AES: Development of unobtrusive seizure-detection devices continues

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AES: Development of unobtrusive seizure-detection devices continues

PHILADELPHIA – Reliable, externally worn seizure-detection devices for epilepsy patients have been eagerly sought but elusive. New results from the pivotal trial of an arm-mounted device that works by analyzing skin electromyography showed promise when tested in 142 adults and children with epilepsy who also underwent video EEG monitoring, Dr. José E. Cavazos reported in a poster at the annual meeting of the American Epilepsy Society.

More than 7,000 hours of simultaneous surface electromyography with the investigational device, worn on the patient’s upper arm, and video EEG monitoring as the gold standard for seizure detection showed that the device correctly identified all 29 generalized tonic-clonic seizures experienced by the 142 patients studied. This level of detection came with a false-positive rate of 1.47 false events during every 24 hours of monitoring, with most of the false positives occurring when the device was being placed or removed.

Dr. José E. Cavazos

The results made Dr. Cavazos hopeful that the Food and Drug Administration would clear the device, the Brain Sentinel Seizure Detection and Warning System, for U.S. marketing in 2016. The FDA first received the marketing-clearance application in late 2014, said Dr. Cavazos, an epileptologist and professor of neurology at the University of Texas Health Science Center in San Antonio.

But Dr. Cavazos also conceded that receiving FDA clearance for U.S. sale of the device is just the next step in an ongoing process to prove its clinical value.

“Currently, clinical decisions for epilepsy patients are often based on patient-reported seizure counts. There is a clear need for objective data on seizure frequency,” something now obtainable only by running an expensive visual-monitoring study, said Dr. Cavazos, who is also founder of and a stockholder in the company that is developing this device. “We definitely need to show in future studies that monitoring [with the worn device] has a positive impact on patient care, by reducing hospitalizations and producing improved patient outcomes,” he said in an interview. “These data may be enough to get regulatory clearance to sell the device, but insurers may not want to reimburse for it until we can prove its value.”

When the device detects a generalized tonic-clonic seizure, it produces an audible alert and also starts recording both surface EMG data and local audible sounds for use in future analysis of the patient’s status. In the study, seizure detection occurred an average of 14 seconds following seizure onset as judged by visual EEG monitoring adjudicated by three epileptologists. The study also included an additional 31 patients who initially entered the study and began wearing the device but did not complete the monitoring protocol because of an adverse effect while wearing the monitor, usually mild or moderate skin irritation.

The results from this study come in a context of extensive research efforts aimed trying to find reliable and unobtrusive methods to quickly detect seizures short of running an observational study. The best results so far have come when using devices that monitor brain EEG signals with electrode-containing caps or implanted electrodes. But patients have voiced substantially reduced interest in having to resort to such stigmatizing methods, noted Dr. Elizabeth Donner during a separate talk at the meeting.

Mitchel L. Zoler/Frontline Medical News
Dr. Elizabeth Donner and Dr. Gregory L. Krauss

“Patients don’t want what looks like an EEG-detection device. We need devices that suit our patients’ needs,” said Dr. Donner, an epileptologist at the Hospital for Sick Children in Toronto. Aside from direct measurement of EEG, other approaches involve measurement of heart rate or movement, she noted.

“There are very good techniques for detecting seizures without using EEG,” said Dr. Gregory L. Krauss, a professor of neurology at Johns Hopkins University in Baltimore who joined Dr. Donner in a discussion of the pros and cons of current methods for seizure detection. He specifically cited a heart-rate based detection scheme reported last year by a Belgian team (Seizure. 2015 Nov;[32]:52-61). But like all detection methods, the heart rate–based approach showed a marked trade-off between sensitivity and specificity: A heart-rate threshold of at least 50% above baseline had a sensitivity of 82% while identifying one false positive every hour. Raising the detection threshold to at least 30% above baseline boosted the sensitivity to 91%, but with the cost of flagging 3.5 false positives each hour.

Dr. Krauss is currently trying to develop a motion-based approach to identifying seizure onset using an Apple watch, He concluded that, as of now, development of seizure-detection devices that do not rely on direct measurement of brain EEG patterns remains a work in progress, with no prospectively collected data, although he made this assessment prior to the poster report by Dr. Cavazos at the meeting.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Reliable, externally worn seizure-detection devices for epilepsy patients have been eagerly sought but elusive. New results from the pivotal trial of an arm-mounted device that works by analyzing skin electromyography showed promise when tested in 142 adults and children with epilepsy who also underwent video EEG monitoring, Dr. José E. Cavazos reported in a poster at the annual meeting of the American Epilepsy Society.

More than 7,000 hours of simultaneous surface electromyography with the investigational device, worn on the patient’s upper arm, and video EEG monitoring as the gold standard for seizure detection showed that the device correctly identified all 29 generalized tonic-clonic seizures experienced by the 142 patients studied. This level of detection came with a false-positive rate of 1.47 false events during every 24 hours of monitoring, with most of the false positives occurring when the device was being placed or removed.

Dr. José E. Cavazos

The results made Dr. Cavazos hopeful that the Food and Drug Administration would clear the device, the Brain Sentinel Seizure Detection and Warning System, for U.S. marketing in 2016. The FDA first received the marketing-clearance application in late 2014, said Dr. Cavazos, an epileptologist and professor of neurology at the University of Texas Health Science Center in San Antonio.

But Dr. Cavazos also conceded that receiving FDA clearance for U.S. sale of the device is just the next step in an ongoing process to prove its clinical value.

“Currently, clinical decisions for epilepsy patients are often based on patient-reported seizure counts. There is a clear need for objective data on seizure frequency,” something now obtainable only by running an expensive visual-monitoring study, said Dr. Cavazos, who is also founder of and a stockholder in the company that is developing this device. “We definitely need to show in future studies that monitoring [with the worn device] has a positive impact on patient care, by reducing hospitalizations and producing improved patient outcomes,” he said in an interview. “These data may be enough to get regulatory clearance to sell the device, but insurers may not want to reimburse for it until we can prove its value.”

When the device detects a generalized tonic-clonic seizure, it produces an audible alert and also starts recording both surface EMG data and local audible sounds for use in future analysis of the patient’s status. In the study, seizure detection occurred an average of 14 seconds following seizure onset as judged by visual EEG monitoring adjudicated by three epileptologists. The study also included an additional 31 patients who initially entered the study and began wearing the device but did not complete the monitoring protocol because of an adverse effect while wearing the monitor, usually mild or moderate skin irritation.

The results from this study come in a context of extensive research efforts aimed trying to find reliable and unobtrusive methods to quickly detect seizures short of running an observational study. The best results so far have come when using devices that monitor brain EEG signals with electrode-containing caps or implanted electrodes. But patients have voiced substantially reduced interest in having to resort to such stigmatizing methods, noted Dr. Elizabeth Donner during a separate talk at the meeting.

Mitchel L. Zoler/Frontline Medical News
Dr. Elizabeth Donner and Dr. Gregory L. Krauss

“Patients don’t want what looks like an EEG-detection device. We need devices that suit our patients’ needs,” said Dr. Donner, an epileptologist at the Hospital for Sick Children in Toronto. Aside from direct measurement of EEG, other approaches involve measurement of heart rate or movement, she noted.

“There are very good techniques for detecting seizures without using EEG,” said Dr. Gregory L. Krauss, a professor of neurology at Johns Hopkins University in Baltimore who joined Dr. Donner in a discussion of the pros and cons of current methods for seizure detection. He specifically cited a heart-rate based detection scheme reported last year by a Belgian team (Seizure. 2015 Nov;[32]:52-61). But like all detection methods, the heart rate–based approach showed a marked trade-off between sensitivity and specificity: A heart-rate threshold of at least 50% above baseline had a sensitivity of 82% while identifying one false positive every hour. Raising the detection threshold to at least 30% above baseline boosted the sensitivity to 91%, but with the cost of flagging 3.5 false positives each hour.

Dr. Krauss is currently trying to develop a motion-based approach to identifying seizure onset using an Apple watch, He concluded that, as of now, development of seizure-detection devices that do not rely on direct measurement of brain EEG patterns remains a work in progress, with no prospectively collected data, although he made this assessment prior to the poster report by Dr. Cavazos at the meeting.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Reliable, externally worn seizure-detection devices for epilepsy patients have been eagerly sought but elusive. New results from the pivotal trial of an arm-mounted device that works by analyzing skin electromyography showed promise when tested in 142 adults and children with epilepsy who also underwent video EEG monitoring, Dr. José E. Cavazos reported in a poster at the annual meeting of the American Epilepsy Society.

More than 7,000 hours of simultaneous surface electromyography with the investigational device, worn on the patient’s upper arm, and video EEG monitoring as the gold standard for seizure detection showed that the device correctly identified all 29 generalized tonic-clonic seizures experienced by the 142 patients studied. This level of detection came with a false-positive rate of 1.47 false events during every 24 hours of monitoring, with most of the false positives occurring when the device was being placed or removed.

Dr. José E. Cavazos

The results made Dr. Cavazos hopeful that the Food and Drug Administration would clear the device, the Brain Sentinel Seizure Detection and Warning System, for U.S. marketing in 2016. The FDA first received the marketing-clearance application in late 2014, said Dr. Cavazos, an epileptologist and professor of neurology at the University of Texas Health Science Center in San Antonio.

But Dr. Cavazos also conceded that receiving FDA clearance for U.S. sale of the device is just the next step in an ongoing process to prove its clinical value.

“Currently, clinical decisions for epilepsy patients are often based on patient-reported seizure counts. There is a clear need for objective data on seizure frequency,” something now obtainable only by running an expensive visual-monitoring study, said Dr. Cavazos, who is also founder of and a stockholder in the company that is developing this device. “We definitely need to show in future studies that monitoring [with the worn device] has a positive impact on patient care, by reducing hospitalizations and producing improved patient outcomes,” he said in an interview. “These data may be enough to get regulatory clearance to sell the device, but insurers may not want to reimburse for it until we can prove its value.”

When the device detects a generalized tonic-clonic seizure, it produces an audible alert and also starts recording both surface EMG data and local audible sounds for use in future analysis of the patient’s status. In the study, seizure detection occurred an average of 14 seconds following seizure onset as judged by visual EEG monitoring adjudicated by three epileptologists. The study also included an additional 31 patients who initially entered the study and began wearing the device but did not complete the monitoring protocol because of an adverse effect while wearing the monitor, usually mild or moderate skin irritation.

The results from this study come in a context of extensive research efforts aimed trying to find reliable and unobtrusive methods to quickly detect seizures short of running an observational study. The best results so far have come when using devices that monitor brain EEG signals with electrode-containing caps or implanted electrodes. But patients have voiced substantially reduced interest in having to resort to such stigmatizing methods, noted Dr. Elizabeth Donner during a separate talk at the meeting.

Mitchel L. Zoler/Frontline Medical News
Dr. Elizabeth Donner and Dr. Gregory L. Krauss

“Patients don’t want what looks like an EEG-detection device. We need devices that suit our patients’ needs,” said Dr. Donner, an epileptologist at the Hospital for Sick Children in Toronto. Aside from direct measurement of EEG, other approaches involve measurement of heart rate or movement, she noted.

“There are very good techniques for detecting seizures without using EEG,” said Dr. Gregory L. Krauss, a professor of neurology at Johns Hopkins University in Baltimore who joined Dr. Donner in a discussion of the pros and cons of current methods for seizure detection. He specifically cited a heart-rate based detection scheme reported last year by a Belgian team (Seizure. 2015 Nov;[32]:52-61). But like all detection methods, the heart rate–based approach showed a marked trade-off between sensitivity and specificity: A heart-rate threshold of at least 50% above baseline had a sensitivity of 82% while identifying one false positive every hour. Raising the detection threshold to at least 30% above baseline boosted the sensitivity to 91%, but with the cost of flagging 3.5 false positives each hour.

Dr. Krauss is currently trying to develop a motion-based approach to identifying seizure onset using an Apple watch, He concluded that, as of now, development of seizure-detection devices that do not rely on direct measurement of brain EEG patterns remains a work in progress, with no prospectively collected data, although he made this assessment prior to the poster report by Dr. Cavazos at the meeting.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Inside the Article

Vitals

Key clinical point: A seizure-detection device worn on the arm showed good sensitivity and reasonable specificity, but no data yet exist on its clinical utility.

Major finding: The Brain Sentinel device had 100% sensitivity while resulting in 1.47 false-positive alarms every 24 hours.

Data source: The pivotal trial for the Brain Sentinel device, which collected detection data from 142 adults and children with a history of seizures.

Disclosures: The study was sponsored by Brain Sentinel, which is developing the device. Dr. Cavazos is a founder of the company, holds stock in the company and is a consultant to the company. Dr. Donner had no disclosures. Dr. Krauss has been a consultant to SK Life Science, Acorda Therapeutics, and Sunovion and has received research support from Upsher-Smith, SK Life Science, UCB, Novartis, and Pfizer.

AES: Seizure freedom attainable for most epilepsy patients

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AES: Seizure freedom attainable for most epilepsy patients

PHILADELPHIA - Fully optimized antiepilepsy therapy that tries at least a couple of well-chosen and properly dosed antiseizure drugs as well as follow-up with nondrug options for patients who are unresponsive to pharmaceuticals seems able to render about 80%-90% of epilepsy patients seizure free, Dr. Cynthia L. Harden said while summing up a session on epilepsy therapy at the annual meeting of the American Epilepsy Society.

Finding an appropriate and effective treatment for each epilepsy patient can be “labor intensive and expensive”; it depends in part on a patient’s mood, psychosocial profile, and willingness to comply with treatment; and it often needs the multidisciplinary expertise found at epilepsy centers. But the optimistic message from contemporary seizure-management is that by using a drug or two and in selected patients surgery, diet, or an implanted device, the vast majority of epilepsy patients can become seizure free, noted Dr. Harden, system director of clinical epilepsy services at the Mount Sinai Health System in New York and cochair of the session.

Mitchel L. Zoler/Frontline Medical News
Dr. Cynthia L. Harden

“How many of your uncontrolled patients can become seizure free with more vigilance and tender loving care?” she asked the large audience as she concluded the session. A significant fraction of uncontrolled patients become seizure free when their drug dosage is increased, another drug is substituted or added, their compliance improves, their depression diminishes, or a patient’s understanding of their epilepsy and treatment increases through education, Dr. Harden said.

Drugs remain the cornerstone of seizure control for epilepsy patients, with at least 22 agents now available for epilepsy treatment, including 13 with U.S. or European (or both) approval for initial monotherapy of epilepsy. In addition, study results have shown several agents – carbamazepine, lamotrigine, levetiracetam, oxcarbazepine, phenytoin, and zonisamide – to be more or less equally effective for treating newly diagnosed focal epilepsy, which means that clinicians must also consider factors beyond just efficacy, such as adverse effects, impact on a specific patient’s comorbidities, interactions with other drugs a patient takes, and ease of use and cost, said Dr. Emilio Perucca, a neurologist and professor of pharmacology at the University of Pavia (Italy). In general, newer antiepilepsy drugs have not been more effective than older drugs, he noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Emilio Perucca

Another feature of drug treatment is that more is usually not better. “Most patients do not need the highest tolerated dosage,” he said, and minimizing dosages to the lowest effective level helps minimize adverse effects. On the other hand, an antiepilepsy drug needs to be administered at an adequate dosage before concluding that it is ineffective for a patient.

Although a majority of patients respond to the first or second antiepilepsy agent they receive, drugs can’t render all patients seizure free. Results from several reported cohorts show that about 45% of patients with newly diagnosed epilepsy respond well to the first drug they receive and about 13% become seizure free on a second drug. After that, the response rates fall off sharply, with roughly 5% of patients responding to a third drug or drug combinations, said Dr. Patrick Kwan, professor and chairman of neurology at the University of Melbourne and head of epilepsy at Royal Melbourne Hospital. “Once a patient has failed two drugs, even if they become seizure free on a subsequent drug, there is a higher rate of relapse,” Dr. Kwan noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Patrick Kwan

In general, 60%-65% of newly diagnosed epilepsy patients become seizure free with drug monotherapy, Dr. Kwan summarized. Epilepsy patients who fail to fully respond to the first two antiepilepsy drugs they receive need “prompt” referral to an epilepsy center. A “substantial proportion” of patients like this can become seizure free by further optimization of the dosage they receive or by addressing compliance issues, Dr. Kwan said. In addition, some patients achieve full or partial seizure freedom through multidrug treatment or with other treatments.

Two-drug combinations have generally been more effective than combinations with three or more drugs, said Dr. Josiane LaJoie, a pediatric neurologist at New York University. “Using three or more drugs probably won’t lead to better control, just more adverse events,” she cautioned. Many published study results have documented successful two-drug combinations, such as lamotrigine and valproate, and valproate and clobazam, to name just two combinations. In addition to looking at combinations with successful track records in published studies, she highlighted the importance of combining drugs with distinct mechanisms of action and avoiding combing drugs with similar adverse-event profiles. Combinations also need to be tailored to each patient’s clinical characteristics, taking possible drug-drug interactions into account, Dr. LaJoie said.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Josiane LaJoie

When drug treatment fails to produce seizure freedom, other options are resective or ablative surgery, diet, or a neurostimulation implant. “At no time in history have we had as many nonpharmacologic treatment options as we have today,” said Dr. Christopher T. Skidmore, a neurologist in the Comprehensive Epilepsy Center at Thomas Jefferson University in Philadelphia. “With diet or neurostimulation, you get seizure reduction without the adverse effects of addition additional drugs.”

Study results with three different diets indicate that they can each produce a roughly 50% cut in seizure rate in about half the patients who adhere to the diet. The ketogenic diet has the longest track record, but with a 90% fat content, it is notoriously difficult to stick with and requires that patients eat meals that often preclude eating with friends or family members or away from home. Adhering to a modified Atkins diet or a low glycemic load diet seems about as effective as a ketogenic diet while offering more food flexibility and a range of foods more compatible with group meals or meals outside the home, Dr. Skidmore said.

Mitchel L. Zoler/Frontline Medical News
Dr. Christopher T. Skidmore

Even though the modified Atkins and low glycemic load diets offer somewhat more flexibility, both remain a “paradigm shift in food consumption,” compared with what most Americans eat, and when compliance is poor they don’t work. “Diet doesn’t work when people cheat,” Dr. Skidmore noted.

Three forms of nerve stimulation have also shown efficacy for seizure reduction, he said: vagal nerve stimulation, responsive neurostimulation, and deep brain stimulation of the anterior nucleus of the thalamus. “All three devices have proven efficacy,” he noted. “Neurostimulation offers an alternative to medical therapy that does not require daily effort and compliance.”

Discussions with patients about diet, neurostimulation, and surgery options allow each patient to decide whether one or more of these might be a good option. “It takes a certain patient to follow a diet or want an implant,” he said. “There is no one right choice. You need to educate patients and help them make their choice,” Dr. Skidmore advised.

Dr. Harmon had no disclosures. Dr. Perucca has served as a consultant to and received honoraria from Biopharma Solutions, GW Pharma, Takeda, Sun Pharma, and UCB Pharma. Dr. Kwan has been a consultant to Eisai and Novartis and has received research funding from UCB. Dr. LaJoie had no disclosures. Dr. Skidmore has been a consultant to Supernus and a site principal investigator for NeuroPace.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA - Fully optimized antiepilepsy therapy that tries at least a couple of well-chosen and properly dosed antiseizure drugs as well as follow-up with nondrug options for patients who are unresponsive to pharmaceuticals seems able to render about 80%-90% of epilepsy patients seizure free, Dr. Cynthia L. Harden said while summing up a session on epilepsy therapy at the annual meeting of the American Epilepsy Society.

Finding an appropriate and effective treatment for each epilepsy patient can be “labor intensive and expensive”; it depends in part on a patient’s mood, psychosocial profile, and willingness to comply with treatment; and it often needs the multidisciplinary expertise found at epilepsy centers. But the optimistic message from contemporary seizure-management is that by using a drug or two and in selected patients surgery, diet, or an implanted device, the vast majority of epilepsy patients can become seizure free, noted Dr. Harden, system director of clinical epilepsy services at the Mount Sinai Health System in New York and cochair of the session.

Mitchel L. Zoler/Frontline Medical News
Dr. Cynthia L. Harden

“How many of your uncontrolled patients can become seizure free with more vigilance and tender loving care?” she asked the large audience as she concluded the session. A significant fraction of uncontrolled patients become seizure free when their drug dosage is increased, another drug is substituted or added, their compliance improves, their depression diminishes, or a patient’s understanding of their epilepsy and treatment increases through education, Dr. Harden said.

Drugs remain the cornerstone of seizure control for epilepsy patients, with at least 22 agents now available for epilepsy treatment, including 13 with U.S. or European (or both) approval for initial monotherapy of epilepsy. In addition, study results have shown several agents – carbamazepine, lamotrigine, levetiracetam, oxcarbazepine, phenytoin, and zonisamide – to be more or less equally effective for treating newly diagnosed focal epilepsy, which means that clinicians must also consider factors beyond just efficacy, such as adverse effects, impact on a specific patient’s comorbidities, interactions with other drugs a patient takes, and ease of use and cost, said Dr. Emilio Perucca, a neurologist and professor of pharmacology at the University of Pavia (Italy). In general, newer antiepilepsy drugs have not been more effective than older drugs, he noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Emilio Perucca

Another feature of drug treatment is that more is usually not better. “Most patients do not need the highest tolerated dosage,” he said, and minimizing dosages to the lowest effective level helps minimize adverse effects. On the other hand, an antiepilepsy drug needs to be administered at an adequate dosage before concluding that it is ineffective for a patient.

Although a majority of patients respond to the first or second antiepilepsy agent they receive, drugs can’t render all patients seizure free. Results from several reported cohorts show that about 45% of patients with newly diagnosed epilepsy respond well to the first drug they receive and about 13% become seizure free on a second drug. After that, the response rates fall off sharply, with roughly 5% of patients responding to a third drug or drug combinations, said Dr. Patrick Kwan, professor and chairman of neurology at the University of Melbourne and head of epilepsy at Royal Melbourne Hospital. “Once a patient has failed two drugs, even if they become seizure free on a subsequent drug, there is a higher rate of relapse,” Dr. Kwan noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Patrick Kwan

In general, 60%-65% of newly diagnosed epilepsy patients become seizure free with drug monotherapy, Dr. Kwan summarized. Epilepsy patients who fail to fully respond to the first two antiepilepsy drugs they receive need “prompt” referral to an epilepsy center. A “substantial proportion” of patients like this can become seizure free by further optimization of the dosage they receive or by addressing compliance issues, Dr. Kwan said. In addition, some patients achieve full or partial seizure freedom through multidrug treatment or with other treatments.

Two-drug combinations have generally been more effective than combinations with three or more drugs, said Dr. Josiane LaJoie, a pediatric neurologist at New York University. “Using three or more drugs probably won’t lead to better control, just more adverse events,” she cautioned. Many published study results have documented successful two-drug combinations, such as lamotrigine and valproate, and valproate and clobazam, to name just two combinations. In addition to looking at combinations with successful track records in published studies, she highlighted the importance of combining drugs with distinct mechanisms of action and avoiding combing drugs with similar adverse-event profiles. Combinations also need to be tailored to each patient’s clinical characteristics, taking possible drug-drug interactions into account, Dr. LaJoie said.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Josiane LaJoie

When drug treatment fails to produce seizure freedom, other options are resective or ablative surgery, diet, or a neurostimulation implant. “At no time in history have we had as many nonpharmacologic treatment options as we have today,” said Dr. Christopher T. Skidmore, a neurologist in the Comprehensive Epilepsy Center at Thomas Jefferson University in Philadelphia. “With diet or neurostimulation, you get seizure reduction without the adverse effects of addition additional drugs.”

Study results with three different diets indicate that they can each produce a roughly 50% cut in seizure rate in about half the patients who adhere to the diet. The ketogenic diet has the longest track record, but with a 90% fat content, it is notoriously difficult to stick with and requires that patients eat meals that often preclude eating with friends or family members or away from home. Adhering to a modified Atkins diet or a low glycemic load diet seems about as effective as a ketogenic diet while offering more food flexibility and a range of foods more compatible with group meals or meals outside the home, Dr. Skidmore said.

Mitchel L. Zoler/Frontline Medical News
Dr. Christopher T. Skidmore

Even though the modified Atkins and low glycemic load diets offer somewhat more flexibility, both remain a “paradigm shift in food consumption,” compared with what most Americans eat, and when compliance is poor they don’t work. “Diet doesn’t work when people cheat,” Dr. Skidmore noted.

Three forms of nerve stimulation have also shown efficacy for seizure reduction, he said: vagal nerve stimulation, responsive neurostimulation, and deep brain stimulation of the anterior nucleus of the thalamus. “All three devices have proven efficacy,” he noted. “Neurostimulation offers an alternative to medical therapy that does not require daily effort and compliance.”

Discussions with patients about diet, neurostimulation, and surgery options allow each patient to decide whether one or more of these might be a good option. “It takes a certain patient to follow a diet or want an implant,” he said. “There is no one right choice. You need to educate patients and help them make their choice,” Dr. Skidmore advised.

Dr. Harmon had no disclosures. Dr. Perucca has served as a consultant to and received honoraria from Biopharma Solutions, GW Pharma, Takeda, Sun Pharma, and UCB Pharma. Dr. Kwan has been a consultant to Eisai and Novartis and has received research funding from UCB. Dr. LaJoie had no disclosures. Dr. Skidmore has been a consultant to Supernus and a site principal investigator for NeuroPace.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA - Fully optimized antiepilepsy therapy that tries at least a couple of well-chosen and properly dosed antiseizure drugs as well as follow-up with nondrug options for patients who are unresponsive to pharmaceuticals seems able to render about 80%-90% of epilepsy patients seizure free, Dr. Cynthia L. Harden said while summing up a session on epilepsy therapy at the annual meeting of the American Epilepsy Society.

Finding an appropriate and effective treatment for each epilepsy patient can be “labor intensive and expensive”; it depends in part on a patient’s mood, psychosocial profile, and willingness to comply with treatment; and it often needs the multidisciplinary expertise found at epilepsy centers. But the optimistic message from contemporary seizure-management is that by using a drug or two and in selected patients surgery, diet, or an implanted device, the vast majority of epilepsy patients can become seizure free, noted Dr. Harden, system director of clinical epilepsy services at the Mount Sinai Health System in New York and cochair of the session.

Mitchel L. Zoler/Frontline Medical News
Dr. Cynthia L. Harden

“How many of your uncontrolled patients can become seizure free with more vigilance and tender loving care?” she asked the large audience as she concluded the session. A significant fraction of uncontrolled patients become seizure free when their drug dosage is increased, another drug is substituted or added, their compliance improves, their depression diminishes, or a patient’s understanding of their epilepsy and treatment increases through education, Dr. Harden said.

Drugs remain the cornerstone of seizure control for epilepsy patients, with at least 22 agents now available for epilepsy treatment, including 13 with U.S. or European (or both) approval for initial monotherapy of epilepsy. In addition, study results have shown several agents – carbamazepine, lamotrigine, levetiracetam, oxcarbazepine, phenytoin, and zonisamide – to be more or less equally effective for treating newly diagnosed focal epilepsy, which means that clinicians must also consider factors beyond just efficacy, such as adverse effects, impact on a specific patient’s comorbidities, interactions with other drugs a patient takes, and ease of use and cost, said Dr. Emilio Perucca, a neurologist and professor of pharmacology at the University of Pavia (Italy). In general, newer antiepilepsy drugs have not been more effective than older drugs, he noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Emilio Perucca

Another feature of drug treatment is that more is usually not better. “Most patients do not need the highest tolerated dosage,” he said, and minimizing dosages to the lowest effective level helps minimize adverse effects. On the other hand, an antiepilepsy drug needs to be administered at an adequate dosage before concluding that it is ineffective for a patient.

Although a majority of patients respond to the first or second antiepilepsy agent they receive, drugs can’t render all patients seizure free. Results from several reported cohorts show that about 45% of patients with newly diagnosed epilepsy respond well to the first drug they receive and about 13% become seizure free on a second drug. After that, the response rates fall off sharply, with roughly 5% of patients responding to a third drug or drug combinations, said Dr. Patrick Kwan, professor and chairman of neurology at the University of Melbourne and head of epilepsy at Royal Melbourne Hospital. “Once a patient has failed two drugs, even if they become seizure free on a subsequent drug, there is a higher rate of relapse,” Dr. Kwan noted.

Mitchel L. Zoler/Frontline Medical News
Dr. Patrick Kwan

In general, 60%-65% of newly diagnosed epilepsy patients become seizure free with drug monotherapy, Dr. Kwan summarized. Epilepsy patients who fail to fully respond to the first two antiepilepsy drugs they receive need “prompt” referral to an epilepsy center. A “substantial proportion” of patients like this can become seizure free by further optimization of the dosage they receive or by addressing compliance issues, Dr. Kwan said. In addition, some patients achieve full or partial seizure freedom through multidrug treatment or with other treatments.

Two-drug combinations have generally been more effective than combinations with three or more drugs, said Dr. Josiane LaJoie, a pediatric neurologist at New York University. “Using three or more drugs probably won’t lead to better control, just more adverse events,” she cautioned. Many published study results have documented successful two-drug combinations, such as lamotrigine and valproate, and valproate and clobazam, to name just two combinations. In addition to looking at combinations with successful track records in published studies, she highlighted the importance of combining drugs with distinct mechanisms of action and avoiding combing drugs with similar adverse-event profiles. Combinations also need to be tailored to each patient’s clinical characteristics, taking possible drug-drug interactions into account, Dr. LaJoie said.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Josiane LaJoie

When drug treatment fails to produce seizure freedom, other options are resective or ablative surgery, diet, or a neurostimulation implant. “At no time in history have we had as many nonpharmacologic treatment options as we have today,” said Dr. Christopher T. Skidmore, a neurologist in the Comprehensive Epilepsy Center at Thomas Jefferson University in Philadelphia. “With diet or neurostimulation, you get seizure reduction without the adverse effects of addition additional drugs.”

Study results with three different diets indicate that they can each produce a roughly 50% cut in seizure rate in about half the patients who adhere to the diet. The ketogenic diet has the longest track record, but with a 90% fat content, it is notoriously difficult to stick with and requires that patients eat meals that often preclude eating with friends or family members or away from home. Adhering to a modified Atkins diet or a low glycemic load diet seems about as effective as a ketogenic diet while offering more food flexibility and a range of foods more compatible with group meals or meals outside the home, Dr. Skidmore said.

Mitchel L. Zoler/Frontline Medical News
Dr. Christopher T. Skidmore

Even though the modified Atkins and low glycemic load diets offer somewhat more flexibility, both remain a “paradigm shift in food consumption,” compared with what most Americans eat, and when compliance is poor they don’t work. “Diet doesn’t work when people cheat,” Dr. Skidmore noted.

Three forms of nerve stimulation have also shown efficacy for seizure reduction, he said: vagal nerve stimulation, responsive neurostimulation, and deep brain stimulation of the anterior nucleus of the thalamus. “All three devices have proven efficacy,” he noted. “Neurostimulation offers an alternative to medical therapy that does not require daily effort and compliance.”

Discussions with patients about diet, neurostimulation, and surgery options allow each patient to decide whether one or more of these might be a good option. “It takes a certain patient to follow a diet or want an implant,” he said. “There is no one right choice. You need to educate patients and help them make their choice,” Dr. Skidmore advised.

Dr. Harmon had no disclosures. Dr. Perucca has served as a consultant to and received honoraria from Biopharma Solutions, GW Pharma, Takeda, Sun Pharma, and UCB Pharma. Dr. Kwan has been a consultant to Eisai and Novartis and has received research funding from UCB. Dr. LaJoie had no disclosures. Dr. Skidmore has been a consultant to Supernus and a site principal investigator for NeuroPace.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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AES: Sparse evidence hints at epilepsy disease modification

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PHILADELPHIA – Tantalizing hints support the possibility that disease modification of epilepsy is possible, but while the best evidence available today for disease modification may be “very encouraging and strongly suggestive,” it also remains low-level evidence drawn from modest numbers of patients, Dr. Andrew J. Cole said during the annual meeting of the American Epilepsy Society.

The upshot is that proving disease modification is feasible for some epilepsy types “stands to be a great challenge for a long time to come,” said Dr. Cole, professor of neurology at Harvard Medical School and director of the epilepsy service at Massachusetts General Hospital, both in Boston.

Mitchel L. Zoler/Frontline Medical News
Dr. Andrew J. Cole

Dr. Cole started by defining disease modification: A treatment that modifies a disease’s expression, course, severity or duration, or modifies comorbidities integral to the disease. These effects need not be mutually exclusive, he added. Another issue about disease modification is that it presumably takes a long time to happen, which makes it harder to recognize. “Disease modification likely happens over the long term, which produces a severe methodological challenge,” Dr. Cole said.

Perhaps the best example of what appears to be disease modification of epilepsy are the long-term outcomes of patients with severe disease – 30 or more seizures a month – who receive long-term treatment with deep brain stimulation (DBS). These patients “seem to get better and better over several years [of treatment], as if their disease was changing,” he said.

For example, both the short- and long-term follow-up of patients enrolled in the Stimulation of the Anterior Nucleus of the Thalamus for Epilepsy (SANTE) trial, which enrolled 157 patients, showed that over time continued DBS linked with a steady decrease in seizure numbers. Recently published long-term follow-up results showed that seizure reduction grew from an average drop of 41% from baseline numbers after 1 year of DBS to an average reduction from baseline of 69% after 5 years (Neurology. 2015 Mar 10;84[10]:1017-25).

A similar pattern of this DBS effect came in 2-year follow-up results from the 191-patient pivotal trial for the responsive neurostimulation system, which showed a 44% reduction, compared with baseline in seizure incidence after 1 year and a 53% reduction after 2 years (Epilepsia. 2014 March;55[3]:432-41). Once again, the findings suggest “a plasticity response and not a purely symptomatic response,” Dr. Cole said.

He also cited findings from two additional, much smaller series of patients who stopped prolonged treatment with DBS and continued to have low seizure rates, compared with the incidence before DBS began. In short, observations from several series of patients who underwent DBS make a “reasonable case for disease modification by suggesting disease modification can occur,” Dr. Cole said.

He cited two additional lines of evidence: a rat model of early treatment for spike-wave epilepsy (Epilepsia. 2008 Mar;49[3]:400-9), and studies of patients with epileptic encephalopathy that have shown associations between early treatment and better cognitive outcomes regardless of the type of treatment patients received (Epilepsia. 2015 Oct;56[10]:1482-5). One limitation of the epileptic encephalopathy examples is the difficulty, if not impossibility. of conducting randomized trials to truly test the hypothesis that treatment can be disease modifying. “The big problem is distinguishing an anticonvulsant effect of treatment from a disease-modifying antiepileptogenic effect,” Dr. Cole said.

He proposed a clinical setting where it’s possible to envision a randomized clinical trial that could test whether a disease-modifying effect occurs: Prophylactic treatment of people who have experienced brain insults known to potentially trigger epilepsy, such as head trauma or stroke. So far, this approach has not been used to test possible disease-modifying treatments. Although such studies are plausible they would also be limited by the number of patients required to produce statistically meaningful results.

Dr. Cole estimated that based on assumptions of epilepsy incidence following various types of brain insults and the possible efficacy of a disease-modifying intervention, such trials could require anywhere from several hundred to several thousand patients, with price tags ranging from more than $10 million to more than $100 million per study. Plus, “even if we had success, [the treatment] would be relevant to a relatively small fraction of patients with epilepsy,” he said.

Dr. Cole said that he has been a consultant to Precisis, NeuroPace, and Nestec.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Tantalizing hints support the possibility that disease modification of epilepsy is possible, but while the best evidence available today for disease modification may be “very encouraging and strongly suggestive,” it also remains low-level evidence drawn from modest numbers of patients, Dr. Andrew J. Cole said during the annual meeting of the American Epilepsy Society.

The upshot is that proving disease modification is feasible for some epilepsy types “stands to be a great challenge for a long time to come,” said Dr. Cole, professor of neurology at Harvard Medical School and director of the epilepsy service at Massachusetts General Hospital, both in Boston.

Mitchel L. Zoler/Frontline Medical News
Dr. Andrew J. Cole

Dr. Cole started by defining disease modification: A treatment that modifies a disease’s expression, course, severity or duration, or modifies comorbidities integral to the disease. These effects need not be mutually exclusive, he added. Another issue about disease modification is that it presumably takes a long time to happen, which makes it harder to recognize. “Disease modification likely happens over the long term, which produces a severe methodological challenge,” Dr. Cole said.

Perhaps the best example of what appears to be disease modification of epilepsy are the long-term outcomes of patients with severe disease – 30 or more seizures a month – who receive long-term treatment with deep brain stimulation (DBS). These patients “seem to get better and better over several years [of treatment], as if their disease was changing,” he said.

For example, both the short- and long-term follow-up of patients enrolled in the Stimulation of the Anterior Nucleus of the Thalamus for Epilepsy (SANTE) trial, which enrolled 157 patients, showed that over time continued DBS linked with a steady decrease in seizure numbers. Recently published long-term follow-up results showed that seizure reduction grew from an average drop of 41% from baseline numbers after 1 year of DBS to an average reduction from baseline of 69% after 5 years (Neurology. 2015 Mar 10;84[10]:1017-25).

A similar pattern of this DBS effect came in 2-year follow-up results from the 191-patient pivotal trial for the responsive neurostimulation system, which showed a 44% reduction, compared with baseline in seizure incidence after 1 year and a 53% reduction after 2 years (Epilepsia. 2014 March;55[3]:432-41). Once again, the findings suggest “a plasticity response and not a purely symptomatic response,” Dr. Cole said.

He also cited findings from two additional, much smaller series of patients who stopped prolonged treatment with DBS and continued to have low seizure rates, compared with the incidence before DBS began. In short, observations from several series of patients who underwent DBS make a “reasonable case for disease modification by suggesting disease modification can occur,” Dr. Cole said.

He cited two additional lines of evidence: a rat model of early treatment for spike-wave epilepsy (Epilepsia. 2008 Mar;49[3]:400-9), and studies of patients with epileptic encephalopathy that have shown associations between early treatment and better cognitive outcomes regardless of the type of treatment patients received (Epilepsia. 2015 Oct;56[10]:1482-5). One limitation of the epileptic encephalopathy examples is the difficulty, if not impossibility. of conducting randomized trials to truly test the hypothesis that treatment can be disease modifying. “The big problem is distinguishing an anticonvulsant effect of treatment from a disease-modifying antiepileptogenic effect,” Dr. Cole said.

He proposed a clinical setting where it’s possible to envision a randomized clinical trial that could test whether a disease-modifying effect occurs: Prophylactic treatment of people who have experienced brain insults known to potentially trigger epilepsy, such as head trauma or stroke. So far, this approach has not been used to test possible disease-modifying treatments. Although such studies are plausible they would also be limited by the number of patients required to produce statistically meaningful results.

Dr. Cole estimated that based on assumptions of epilepsy incidence following various types of brain insults and the possible efficacy of a disease-modifying intervention, such trials could require anywhere from several hundred to several thousand patients, with price tags ranging from more than $10 million to more than $100 million per study. Plus, “even if we had success, [the treatment] would be relevant to a relatively small fraction of patients with epilepsy,” he said.

Dr. Cole said that he has been a consultant to Precisis, NeuroPace, and Nestec.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Tantalizing hints support the possibility that disease modification of epilepsy is possible, but while the best evidence available today for disease modification may be “very encouraging and strongly suggestive,” it also remains low-level evidence drawn from modest numbers of patients, Dr. Andrew J. Cole said during the annual meeting of the American Epilepsy Society.

The upshot is that proving disease modification is feasible for some epilepsy types “stands to be a great challenge for a long time to come,” said Dr. Cole, professor of neurology at Harvard Medical School and director of the epilepsy service at Massachusetts General Hospital, both in Boston.

Mitchel L. Zoler/Frontline Medical News
Dr. Andrew J. Cole

Dr. Cole started by defining disease modification: A treatment that modifies a disease’s expression, course, severity or duration, or modifies comorbidities integral to the disease. These effects need not be mutually exclusive, he added. Another issue about disease modification is that it presumably takes a long time to happen, which makes it harder to recognize. “Disease modification likely happens over the long term, which produces a severe methodological challenge,” Dr. Cole said.

Perhaps the best example of what appears to be disease modification of epilepsy are the long-term outcomes of patients with severe disease – 30 or more seizures a month – who receive long-term treatment with deep brain stimulation (DBS). These patients “seem to get better and better over several years [of treatment], as if their disease was changing,” he said.

For example, both the short- and long-term follow-up of patients enrolled in the Stimulation of the Anterior Nucleus of the Thalamus for Epilepsy (SANTE) trial, which enrolled 157 patients, showed that over time continued DBS linked with a steady decrease in seizure numbers. Recently published long-term follow-up results showed that seizure reduction grew from an average drop of 41% from baseline numbers after 1 year of DBS to an average reduction from baseline of 69% after 5 years (Neurology. 2015 Mar 10;84[10]:1017-25).

A similar pattern of this DBS effect came in 2-year follow-up results from the 191-patient pivotal trial for the responsive neurostimulation system, which showed a 44% reduction, compared with baseline in seizure incidence after 1 year and a 53% reduction after 2 years (Epilepsia. 2014 March;55[3]:432-41). Once again, the findings suggest “a plasticity response and not a purely symptomatic response,” Dr. Cole said.

He also cited findings from two additional, much smaller series of patients who stopped prolonged treatment with DBS and continued to have low seizure rates, compared with the incidence before DBS began. In short, observations from several series of patients who underwent DBS make a “reasonable case for disease modification by suggesting disease modification can occur,” Dr. Cole said.

He cited two additional lines of evidence: a rat model of early treatment for spike-wave epilepsy (Epilepsia. 2008 Mar;49[3]:400-9), and studies of patients with epileptic encephalopathy that have shown associations between early treatment and better cognitive outcomes regardless of the type of treatment patients received (Epilepsia. 2015 Oct;56[10]:1482-5). One limitation of the epileptic encephalopathy examples is the difficulty, if not impossibility. of conducting randomized trials to truly test the hypothesis that treatment can be disease modifying. “The big problem is distinguishing an anticonvulsant effect of treatment from a disease-modifying antiepileptogenic effect,” Dr. Cole said.

He proposed a clinical setting where it’s possible to envision a randomized clinical trial that could test whether a disease-modifying effect occurs: Prophylactic treatment of people who have experienced brain insults known to potentially trigger epilepsy, such as head trauma or stroke. So far, this approach has not been used to test possible disease-modifying treatments. Although such studies are plausible they would also be limited by the number of patients required to produce statistically meaningful results.

Dr. Cole estimated that based on assumptions of epilepsy incidence following various types of brain insults and the possible efficacy of a disease-modifying intervention, such trials could require anywhere from several hundred to several thousand patients, with price tags ranging from more than $10 million to more than $100 million per study. Plus, “even if we had success, [the treatment] would be relevant to a relatively small fraction of patients with epilepsy,” he said.

Dr. Cole said that he has been a consultant to Precisis, NeuroPace, and Nestec.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Good luck convincing patients that generics equal brand-name drugs

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Generic drugs have long carried a stigma for at least some people. Patients sometimes feel scared and shortchanged when prescribed them, and some physicians have been wary of their safety and efficacy, compared with brand-name counterparts.

This fall, results appeared from a trio of prospective, randomized studies that compared several generic forms of the antiepileptic drug lamotrigine against the brand-name compound, Lamictal, in patients with epilepsy. As reported earlier this month in a special session at the annual meeting of the American Epilepsy Society, and as I wrote up in a news article, the findings from all three studies consistently and clearly showed that the generic lamotrigine products tested in these three studies all performed identically to Lamictal by both their pharmacokinetic profiles and in their clinical safety and efficacy.

Giorgiogp2/Wikimedia Commons/CC BY-SA 3.0
Lamotrigine's chemical structure

A critic could quibble that the three studies involved relatively small numbers of patients (they included 34-48 subjects), that the treatment times were relatively brief (a matter of a few weeks), and the investigations were limited to just lamotrigine. But the neurologists who reported these findings, a pair of Food and Drug Administration staffers who deal with generics and spoke at the session, and two pharmacy researchers who also participated in the panel all agreed that these groundbreaking studies establish an unprecedented level of confidence in not just the generic products tested but for generic drugs in general.

As Dr. Michael Privitera, director of the Epilepsy Center at the University of Cincinnati and a lead investigator for two of the three studies, told me, controlling seizures in epilepsy patients is a stringent test of drug efficacy and similarity. If generic forms of lamotrigine behave indistinguishably from Lamictal, then it’s very reasonable to expect that virtually any generic form of any brand-name drug used in medicine is also a good mimic if it recently passed FDA muster. His only caveat was selected drugs with very unusual pharmacokinetic properties, such as phenytoin – another antiepileptic drug, which has saturation kinetics making it a special case that requires additional, customized testing to prove equivalence between the generic and brand-name form.

But as he and others at the session highlighted, equivalent pharmacologic properties of generic and brand-name forms of a drug tell just part of the story. They may act the same once inside patients’ bodies, but what’s also important is how patients regard these drugs from the neck up. Psychological factors play a role in how patients perceive and use different forms of chemically identical products. Differences in pill size, shape, and color can confuse patients, and just knowing that a drug is a generic could possibly trigger anxiety in a patient that might perhaps produce a seizure or disrupt their pill-taking behavior. Several clinicians at the session spoke of certain patients who have begged them to specify the brand-name drug on their prescriptions. On the other hand, a generic’s lower price often encourages more conscientious use, a phenomenon documented in a database review reported at the session by pharmacoepidemiologist Joshua J. Gagne, Pharm.D.

Madison Avenue has known for years that function and utility tell just part of the story when it comes to consumer goods. A Kia may be just as durable and effective for transporting someone as a Mercedes or BMW, but cheap isn’t always what a consumer wants or feels comfortable with. Generics that work indistinguishably from brand drugs are certainly attractive for the U.S. health care system and the majority of the American public, but the concept that generic is best will be tough to sell to everyone.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Generic drugs have long carried a stigma for at least some people. Patients sometimes feel scared and shortchanged when prescribed them, and some physicians have been wary of their safety and efficacy, compared with brand-name counterparts.

This fall, results appeared from a trio of prospective, randomized studies that compared several generic forms of the antiepileptic drug lamotrigine against the brand-name compound, Lamictal, in patients with epilepsy. As reported earlier this month in a special session at the annual meeting of the American Epilepsy Society, and as I wrote up in a news article, the findings from all three studies consistently and clearly showed that the generic lamotrigine products tested in these three studies all performed identically to Lamictal by both their pharmacokinetic profiles and in their clinical safety and efficacy.

Giorgiogp2/Wikimedia Commons/CC BY-SA 3.0
Lamotrigine's chemical structure

A critic could quibble that the three studies involved relatively small numbers of patients (they included 34-48 subjects), that the treatment times were relatively brief (a matter of a few weeks), and the investigations were limited to just lamotrigine. But the neurologists who reported these findings, a pair of Food and Drug Administration staffers who deal with generics and spoke at the session, and two pharmacy researchers who also participated in the panel all agreed that these groundbreaking studies establish an unprecedented level of confidence in not just the generic products tested but for generic drugs in general.

As Dr. Michael Privitera, director of the Epilepsy Center at the University of Cincinnati and a lead investigator for two of the three studies, told me, controlling seizures in epilepsy patients is a stringent test of drug efficacy and similarity. If generic forms of lamotrigine behave indistinguishably from Lamictal, then it’s very reasonable to expect that virtually any generic form of any brand-name drug used in medicine is also a good mimic if it recently passed FDA muster. His only caveat was selected drugs with very unusual pharmacokinetic properties, such as phenytoin – another antiepileptic drug, which has saturation kinetics making it a special case that requires additional, customized testing to prove equivalence between the generic and brand-name form.

But as he and others at the session highlighted, equivalent pharmacologic properties of generic and brand-name forms of a drug tell just part of the story. They may act the same once inside patients’ bodies, but what’s also important is how patients regard these drugs from the neck up. Psychological factors play a role in how patients perceive and use different forms of chemically identical products. Differences in pill size, shape, and color can confuse patients, and just knowing that a drug is a generic could possibly trigger anxiety in a patient that might perhaps produce a seizure or disrupt their pill-taking behavior. Several clinicians at the session spoke of certain patients who have begged them to specify the brand-name drug on their prescriptions. On the other hand, a generic’s lower price often encourages more conscientious use, a phenomenon documented in a database review reported at the session by pharmacoepidemiologist Joshua J. Gagne, Pharm.D.

Madison Avenue has known for years that function and utility tell just part of the story when it comes to consumer goods. A Kia may be just as durable and effective for transporting someone as a Mercedes or BMW, but cheap isn’t always what a consumer wants or feels comfortable with. Generics that work indistinguishably from brand drugs are certainly attractive for the U.S. health care system and the majority of the American public, but the concept that generic is best will be tough to sell to everyone.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

Generic drugs have long carried a stigma for at least some people. Patients sometimes feel scared and shortchanged when prescribed them, and some physicians have been wary of their safety and efficacy, compared with brand-name counterparts.

This fall, results appeared from a trio of prospective, randomized studies that compared several generic forms of the antiepileptic drug lamotrigine against the brand-name compound, Lamictal, in patients with epilepsy. As reported earlier this month in a special session at the annual meeting of the American Epilepsy Society, and as I wrote up in a news article, the findings from all three studies consistently and clearly showed that the generic lamotrigine products tested in these three studies all performed identically to Lamictal by both their pharmacokinetic profiles and in their clinical safety and efficacy.

Giorgiogp2/Wikimedia Commons/CC BY-SA 3.0
Lamotrigine's chemical structure

A critic could quibble that the three studies involved relatively small numbers of patients (they included 34-48 subjects), that the treatment times were relatively brief (a matter of a few weeks), and the investigations were limited to just lamotrigine. But the neurologists who reported these findings, a pair of Food and Drug Administration staffers who deal with generics and spoke at the session, and two pharmacy researchers who also participated in the panel all agreed that these groundbreaking studies establish an unprecedented level of confidence in not just the generic products tested but for generic drugs in general.

As Dr. Michael Privitera, director of the Epilepsy Center at the University of Cincinnati and a lead investigator for two of the three studies, told me, controlling seizures in epilepsy patients is a stringent test of drug efficacy and similarity. If generic forms of lamotrigine behave indistinguishably from Lamictal, then it’s very reasonable to expect that virtually any generic form of any brand-name drug used in medicine is also a good mimic if it recently passed FDA muster. His only caveat was selected drugs with very unusual pharmacokinetic properties, such as phenytoin – another antiepileptic drug, which has saturation kinetics making it a special case that requires additional, customized testing to prove equivalence between the generic and brand-name form.

But as he and others at the session highlighted, equivalent pharmacologic properties of generic and brand-name forms of a drug tell just part of the story. They may act the same once inside patients’ bodies, but what’s also important is how patients regard these drugs from the neck up. Psychological factors play a role in how patients perceive and use different forms of chemically identical products. Differences in pill size, shape, and color can confuse patients, and just knowing that a drug is a generic could possibly trigger anxiety in a patient that might perhaps produce a seizure or disrupt their pill-taking behavior. Several clinicians at the session spoke of certain patients who have begged them to specify the brand-name drug on their prescriptions. On the other hand, a generic’s lower price often encourages more conscientious use, a phenomenon documented in a database review reported at the session by pharmacoepidemiologist Joshua J. Gagne, Pharm.D.

Madison Avenue has known for years that function and utility tell just part of the story when it comes to consumer goods. A Kia may be just as durable and effective for transporting someone as a Mercedes or BMW, but cheap isn’t always what a consumer wants or feels comfortable with. Generics that work indistinguishably from brand drugs are certainly attractive for the U.S. health care system and the majority of the American public, but the concept that generic is best will be tough to sell to everyone.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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AES: Three studies show generic lamotrigine equals Lamictal

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PHILADELPHIA – Several different generic lamotrigine products proved pharmacologically and clinically equivalent to Lamictal, the brand-name, reference form of lamotrigine, in three separate, prospective, randomized trials run by two independent groups. These results that should lay to rest lingering concerns by physicians and patients that generic lamotrigine poses any risk to patients, agreed a panel of experts speaking at a session at the annual meeting of the American Epilepsy Society.

The findings, which confirmed the standards now set by the Food and Drug Administration for deeming generic products equivalent to their reference product, should also reassure physicians and patients more broadly about the reliability of the generic forms of most other antiepileptic drugs as well as generic drugs used for virtually all indications across the range of medical practice, the panelists said.

The results of these three new studies “show that generic drugs have the same quality as the reference-listed drugs in patients with epilepsy,” said Dr. Wenlei Jiang, acting deputy director of the FDA’s Office of Research Standards and Office of Generic Drugs. Dr. Jiang coauthored one of the new studies.

Mitchel L. Zoler/Frontline Medical News
Dr. Michel J. Berg (left) and Dr. Michael Privitera

“We were a skeptical group going into our studies,” said Dr. Michael Privitera, coprincipal investigator for the other two new studies. “We were not sure that these drugs [brand-name lamotrigine and various generic products] were really the same. We were shocked at how equivalent they were. It wasn’t that the differences [among their pharmacokinetic profiles] were small; it’s that there was no difference. We could not see any difference,” said Dr. Privitera, professor of neurology and director of the Epilepsy Center at the University of Cincinnati.

“We chose to study lamotrigine because there had been a lot of complaints [about the generic products] and because it is a drug that is very susceptible to drug-drug interactions. There is no reason I can think of why what we found would not extend to all antiepileptic drugs except for phenytoin, which has saturation kinetics and the way the FDA tests drugs in a single-dose study is not appropriate for drugs with saturation kinetics,” Dr. Privitera said in an interview. The implications of the new findings also extend beyond just drugs for epilepsy or other neurologic conditions, he added.

“When you have a very complicated disorder like epilepsy, which has the possibility for drug-drug interactions, and we could show this much quality” in the generic products, it has implications for the entire universe of generic drugs that show equivalence in FDA-mandated testing, Dr. Privitera said.

Randomized trials in epilepsy patients

One of the two studies run by Dr. Privitera and his associates used a single-dose format, and the second used a chronic-dosage format.

The EQUIGEN (Equivalence Among Antiepileptic Drug Generic and Brand Products in People With Epilepsy) Single Dose Study enrolled 48 epilepsy patients at any of six U.S. centers. All patients were on an antiepileptic drug other than lamotrigine, and the researchers randomized them to receive single doses of the brand-name reference form of lamotrigine (Lamictal), or either of two generic forms of lamotrigine. Patients received single dosages of each of the three study drugs with a 12-23 day washout period separating each dose (the preferred washout interval was 14 days), with the patients and researchers blinded to which specific product was administered at any time. The researchers selected the two FDA-approved generic products with the most widely divergent profiles based on in vitro dissolution testing and prior pharmacokinetic data supplied to the FDA. Forty-five patients received the scheduled two doses (on two different occasions) of each drug, a total of six test doses administered. The remaining three patients received a single dose of each of the three tested products.

All three products resulted in essentially superimposed concentration-time curves and area under the curve measures with no outliers or serious adverse events seen, Dr. Privitera and his associates reported in a poster presented at the meeting as well as during the session.

The EQUIGEN Chronic Dose Study compared the pharmacokinetic patterns after chronic dosing for 2 weeks with one of the two most disparate lamotrigine generic products. The study enrolled 35 patients with epilepsy at any of six U.S. centers, and 33 patients completed all four treatment periods, which involved a repeated crossover between the two study products. Patients received lamotrigine twice daily and could be on additional antiepileptic drugs or monotherapy; six patients received concomitant enzyme-inducing antiepileptic drugs during the study. The results showed that the area under the curve for both products had 90% confidence intervals of 98%-103%, compared with Lamictal, and they both had a 90% confidence interval for peak plasma concentration of 99%-105%, Dr. Privitera and his associates reported at the session. None of the enrolled patients showed unexpected adverse events, and the two generics produced similar adverse-event profiles.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Wenlei Jiang (left) and Dr. Tricia Y. Ting

The third study, BEEP (Bioequivalence in Epilepsy Patients) ran at the University of Maryland, Baltimore, and the results appeared in a journal article published in September (Epilepsia. 2015 Sept;56[9]:1415-24). This study enrolled 34 “generic brittle” epilepsy patients, which meant they had already shown signs of possible sensitivity to switching from Lamictal to generic lamotrigine. The study randomized patients to four consecutive 2-week periods of treatment with either the brand-name or a generic lamotrigine product in a crossover design that was then repeated, and each patient underwent a 12-hour pharmacokinetic analysis after they reached a steady-state drug level with 2 weeks of treatment. The results showed a tight match for both the area under the curve and peak plasma concentration for the generic and brand drugs, said Dr. Tricia Y. Ting, lead investigator for the study and a neurologist and epilepsy specialist at the University of Maryland Medical Center in Baltimore.

“The results could not have been more beautiful. We were quite surprised at how close the generic and brand products were” in their steady-state pharmacokinetic profiles, Dr. Ting said during the session.

The results of the three studies, while reassuring, raise questions as to why some patients nevertheless report problems while taking generic products, noted Dr. Ting. “We need to look outside of bioequivalence, and focus instead on issues such as patient expectations,” she said.

Patient factors

Dr. Joshua J. Gagne, a pharmacoepidemiologist at Brigham and Women’s Hospital in Boston, discussed the role of patient expectations and other patient-specific factors that can affect the safety and efficacy of generic products. He noted that patients can be confused by generic pills that do not have the same size, shape, or color as their brand-name counterparts. “Variations in appearance with generic antiepilepsy drugs is a real problem and may be a barrier to adherence,” he said. In addition, “patients’ out of pocket costs are important drivers of antiepileptic drug adherence,” and may act in favor of generics, he said.

Mitchel L. Zoler/Frontline Medical News
Dr. Joshua J. Gagne

He documented this potential effect in a recent study he published and also summarized while speaking during the session. Dr. Gagne and his associates used a database of more than 19,000 U.S. Medicare patients with epilepsy who began treatment with an antiepileptic drug. The researchers used propensity scoring to match a subset from among the 18,306 patients who started on a generic drug and the 1,454 patients who started on a brand-name drug. In the matched subgroups, those on a generic went an average of 138 days before having a 14-day gap in treatment, compared with an average 124 days until a 14-day treatment gap occurred among those on a branded drug. This difference in adherence linked with a significant difference in seizure-related hospitalizations, experienced by 47 patients who started on a branded drug and in 31 of those who started on a generic. This calculated out to a statistically significant relative risk reduction of more than 50% (Epilepsy Behavior. 2015 Nov;52[part A]:14-8).

Often it is the physician that’s to blame when patients lack trust in a generic drug, noted Dr. Michel J. Berg, a neurologist at the University of Rochester (N.Y.) and coprincipal investigator on the two EQUIGEN studies. “If physicians are confident [in generics] then patients will rely on the physician’s expert opinion,” Dr. Berg said during a panel discussion of these studies during the session.

Patients and physicians also need to realize that today’s generics are often not the same products that they were years ago. The FDA has “encouraged manufacturers to move from ’quality by testing’ to ‘quality by design,’ which has resulted in better products,” stressed Dr. Jiang.

Dr. Privitera agreed. “A lot of the fear about generics was generated 20 or more years ago, when the generic quality was not as good. There were a lot of scary stories out there. Today, with quality by design, manufacturers don’t just try to get their generic in a target range but they do multiple tests earlier in the [generic development] process so that by the time they get to clinical testing they already have a drug that is really tight.”

Members of the audience at the session who commented during the discussion period usually agreed that the new data reported for lamotrigine convinced them of the quality of modern generics. “There has been discomfort with generics, but now we have the data that they are effective and safe,” commented Dr. Mark C. Spitz, professor of neurology and head of the Adult Comprehensive Epilepsy Program at the University of Colorado at Denver, Aurora, who spoke from the floor. “These new data will make a big difference in how epileptologists will practice,” Dr. Spitz predicted.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Several different generic lamotrigine products proved pharmacologically and clinically equivalent to Lamictal, the brand-name, reference form of lamotrigine, in three separate, prospective, randomized trials run by two independent groups. These results that should lay to rest lingering concerns by physicians and patients that generic lamotrigine poses any risk to patients, agreed a panel of experts speaking at a session at the annual meeting of the American Epilepsy Society.

The findings, which confirmed the standards now set by the Food and Drug Administration for deeming generic products equivalent to their reference product, should also reassure physicians and patients more broadly about the reliability of the generic forms of most other antiepileptic drugs as well as generic drugs used for virtually all indications across the range of medical practice, the panelists said.

The results of these three new studies “show that generic drugs have the same quality as the reference-listed drugs in patients with epilepsy,” said Dr. Wenlei Jiang, acting deputy director of the FDA’s Office of Research Standards and Office of Generic Drugs. Dr. Jiang coauthored one of the new studies.

Mitchel L. Zoler/Frontline Medical News
Dr. Michel J. Berg (left) and Dr. Michael Privitera

“We were a skeptical group going into our studies,” said Dr. Michael Privitera, coprincipal investigator for the other two new studies. “We were not sure that these drugs [brand-name lamotrigine and various generic products] were really the same. We were shocked at how equivalent they were. It wasn’t that the differences [among their pharmacokinetic profiles] were small; it’s that there was no difference. We could not see any difference,” said Dr. Privitera, professor of neurology and director of the Epilepsy Center at the University of Cincinnati.

“We chose to study lamotrigine because there had been a lot of complaints [about the generic products] and because it is a drug that is very susceptible to drug-drug interactions. There is no reason I can think of why what we found would not extend to all antiepileptic drugs except for phenytoin, which has saturation kinetics and the way the FDA tests drugs in a single-dose study is not appropriate for drugs with saturation kinetics,” Dr. Privitera said in an interview. The implications of the new findings also extend beyond just drugs for epilepsy or other neurologic conditions, he added.

“When you have a very complicated disorder like epilepsy, which has the possibility for drug-drug interactions, and we could show this much quality” in the generic products, it has implications for the entire universe of generic drugs that show equivalence in FDA-mandated testing, Dr. Privitera said.

Randomized trials in epilepsy patients

One of the two studies run by Dr. Privitera and his associates used a single-dose format, and the second used a chronic-dosage format.

The EQUIGEN (Equivalence Among Antiepileptic Drug Generic and Brand Products in People With Epilepsy) Single Dose Study enrolled 48 epilepsy patients at any of six U.S. centers. All patients were on an antiepileptic drug other than lamotrigine, and the researchers randomized them to receive single doses of the brand-name reference form of lamotrigine (Lamictal), or either of two generic forms of lamotrigine. Patients received single dosages of each of the three study drugs with a 12-23 day washout period separating each dose (the preferred washout interval was 14 days), with the patients and researchers blinded to which specific product was administered at any time. The researchers selected the two FDA-approved generic products with the most widely divergent profiles based on in vitro dissolution testing and prior pharmacokinetic data supplied to the FDA. Forty-five patients received the scheduled two doses (on two different occasions) of each drug, a total of six test doses administered. The remaining three patients received a single dose of each of the three tested products.

All three products resulted in essentially superimposed concentration-time curves and area under the curve measures with no outliers or serious adverse events seen, Dr. Privitera and his associates reported in a poster presented at the meeting as well as during the session.

The EQUIGEN Chronic Dose Study compared the pharmacokinetic patterns after chronic dosing for 2 weeks with one of the two most disparate lamotrigine generic products. The study enrolled 35 patients with epilepsy at any of six U.S. centers, and 33 patients completed all four treatment periods, which involved a repeated crossover between the two study products. Patients received lamotrigine twice daily and could be on additional antiepileptic drugs or monotherapy; six patients received concomitant enzyme-inducing antiepileptic drugs during the study. The results showed that the area under the curve for both products had 90% confidence intervals of 98%-103%, compared with Lamictal, and they both had a 90% confidence interval for peak plasma concentration of 99%-105%, Dr. Privitera and his associates reported at the session. None of the enrolled patients showed unexpected adverse events, and the two generics produced similar adverse-event profiles.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Wenlei Jiang (left) and Dr. Tricia Y. Ting

The third study, BEEP (Bioequivalence in Epilepsy Patients) ran at the University of Maryland, Baltimore, and the results appeared in a journal article published in September (Epilepsia. 2015 Sept;56[9]:1415-24). This study enrolled 34 “generic brittle” epilepsy patients, which meant they had already shown signs of possible sensitivity to switching from Lamictal to generic lamotrigine. The study randomized patients to four consecutive 2-week periods of treatment with either the brand-name or a generic lamotrigine product in a crossover design that was then repeated, and each patient underwent a 12-hour pharmacokinetic analysis after they reached a steady-state drug level with 2 weeks of treatment. The results showed a tight match for both the area under the curve and peak plasma concentration for the generic and brand drugs, said Dr. Tricia Y. Ting, lead investigator for the study and a neurologist and epilepsy specialist at the University of Maryland Medical Center in Baltimore.

“The results could not have been more beautiful. We were quite surprised at how close the generic and brand products were” in their steady-state pharmacokinetic profiles, Dr. Ting said during the session.

The results of the three studies, while reassuring, raise questions as to why some patients nevertheless report problems while taking generic products, noted Dr. Ting. “We need to look outside of bioequivalence, and focus instead on issues such as patient expectations,” she said.

Patient factors

Dr. Joshua J. Gagne, a pharmacoepidemiologist at Brigham and Women’s Hospital in Boston, discussed the role of patient expectations and other patient-specific factors that can affect the safety and efficacy of generic products. He noted that patients can be confused by generic pills that do not have the same size, shape, or color as their brand-name counterparts. “Variations in appearance with generic antiepilepsy drugs is a real problem and may be a barrier to adherence,” he said. In addition, “patients’ out of pocket costs are important drivers of antiepileptic drug adherence,” and may act in favor of generics, he said.

Mitchel L. Zoler/Frontline Medical News
Dr. Joshua J. Gagne

He documented this potential effect in a recent study he published and also summarized while speaking during the session. Dr. Gagne and his associates used a database of more than 19,000 U.S. Medicare patients with epilepsy who began treatment with an antiepileptic drug. The researchers used propensity scoring to match a subset from among the 18,306 patients who started on a generic drug and the 1,454 patients who started on a brand-name drug. In the matched subgroups, those on a generic went an average of 138 days before having a 14-day gap in treatment, compared with an average 124 days until a 14-day treatment gap occurred among those on a branded drug. This difference in adherence linked with a significant difference in seizure-related hospitalizations, experienced by 47 patients who started on a branded drug and in 31 of those who started on a generic. This calculated out to a statistically significant relative risk reduction of more than 50% (Epilepsy Behavior. 2015 Nov;52[part A]:14-8).

Often it is the physician that’s to blame when patients lack trust in a generic drug, noted Dr. Michel J. Berg, a neurologist at the University of Rochester (N.Y.) and coprincipal investigator on the two EQUIGEN studies. “If physicians are confident [in generics] then patients will rely on the physician’s expert opinion,” Dr. Berg said during a panel discussion of these studies during the session.

Patients and physicians also need to realize that today’s generics are often not the same products that they were years ago. The FDA has “encouraged manufacturers to move from ’quality by testing’ to ‘quality by design,’ which has resulted in better products,” stressed Dr. Jiang.

Dr. Privitera agreed. “A lot of the fear about generics was generated 20 or more years ago, when the generic quality was not as good. There were a lot of scary stories out there. Today, with quality by design, manufacturers don’t just try to get their generic in a target range but they do multiple tests earlier in the [generic development] process so that by the time they get to clinical testing they already have a drug that is really tight.”

Members of the audience at the session who commented during the discussion period usually agreed that the new data reported for lamotrigine convinced them of the quality of modern generics. “There has been discomfort with generics, but now we have the data that they are effective and safe,” commented Dr. Mark C. Spitz, professor of neurology and head of the Adult Comprehensive Epilepsy Program at the University of Colorado at Denver, Aurora, who spoke from the floor. “These new data will make a big difference in how epileptologists will practice,” Dr. Spitz predicted.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Several different generic lamotrigine products proved pharmacologically and clinically equivalent to Lamictal, the brand-name, reference form of lamotrigine, in three separate, prospective, randomized trials run by two independent groups. These results that should lay to rest lingering concerns by physicians and patients that generic lamotrigine poses any risk to patients, agreed a panel of experts speaking at a session at the annual meeting of the American Epilepsy Society.

The findings, which confirmed the standards now set by the Food and Drug Administration for deeming generic products equivalent to their reference product, should also reassure physicians and patients more broadly about the reliability of the generic forms of most other antiepileptic drugs as well as generic drugs used for virtually all indications across the range of medical practice, the panelists said.

The results of these three new studies “show that generic drugs have the same quality as the reference-listed drugs in patients with epilepsy,” said Dr. Wenlei Jiang, acting deputy director of the FDA’s Office of Research Standards and Office of Generic Drugs. Dr. Jiang coauthored one of the new studies.

Mitchel L. Zoler/Frontline Medical News
Dr. Michel J. Berg (left) and Dr. Michael Privitera

“We were a skeptical group going into our studies,” said Dr. Michael Privitera, coprincipal investigator for the other two new studies. “We were not sure that these drugs [brand-name lamotrigine and various generic products] were really the same. We were shocked at how equivalent they were. It wasn’t that the differences [among their pharmacokinetic profiles] were small; it’s that there was no difference. We could not see any difference,” said Dr. Privitera, professor of neurology and director of the Epilepsy Center at the University of Cincinnati.

“We chose to study lamotrigine because there had been a lot of complaints [about the generic products] and because it is a drug that is very susceptible to drug-drug interactions. There is no reason I can think of why what we found would not extend to all antiepileptic drugs except for phenytoin, which has saturation kinetics and the way the FDA tests drugs in a single-dose study is not appropriate for drugs with saturation kinetics,” Dr. Privitera said in an interview. The implications of the new findings also extend beyond just drugs for epilepsy or other neurologic conditions, he added.

“When you have a very complicated disorder like epilepsy, which has the possibility for drug-drug interactions, and we could show this much quality” in the generic products, it has implications for the entire universe of generic drugs that show equivalence in FDA-mandated testing, Dr. Privitera said.

Randomized trials in epilepsy patients

One of the two studies run by Dr. Privitera and his associates used a single-dose format, and the second used a chronic-dosage format.

The EQUIGEN (Equivalence Among Antiepileptic Drug Generic and Brand Products in People With Epilepsy) Single Dose Study enrolled 48 epilepsy patients at any of six U.S. centers. All patients were on an antiepileptic drug other than lamotrigine, and the researchers randomized them to receive single doses of the brand-name reference form of lamotrigine (Lamictal), or either of two generic forms of lamotrigine. Patients received single dosages of each of the three study drugs with a 12-23 day washout period separating each dose (the preferred washout interval was 14 days), with the patients and researchers blinded to which specific product was administered at any time. The researchers selected the two FDA-approved generic products with the most widely divergent profiles based on in vitro dissolution testing and prior pharmacokinetic data supplied to the FDA. Forty-five patients received the scheduled two doses (on two different occasions) of each drug, a total of six test doses administered. The remaining three patients received a single dose of each of the three tested products.

All three products resulted in essentially superimposed concentration-time curves and area under the curve measures with no outliers or serious adverse events seen, Dr. Privitera and his associates reported in a poster presented at the meeting as well as during the session.

The EQUIGEN Chronic Dose Study compared the pharmacokinetic patterns after chronic dosing for 2 weeks with one of the two most disparate lamotrigine generic products. The study enrolled 35 patients with epilepsy at any of six U.S. centers, and 33 patients completed all four treatment periods, which involved a repeated crossover between the two study products. Patients received lamotrigine twice daily and could be on additional antiepileptic drugs or monotherapy; six patients received concomitant enzyme-inducing antiepileptic drugs during the study. The results showed that the area under the curve for both products had 90% confidence intervals of 98%-103%, compared with Lamictal, and they both had a 90% confidence interval for peak plasma concentration of 99%-105%, Dr. Privitera and his associates reported at the session. None of the enrolled patients showed unexpected adverse events, and the two generics produced similar adverse-event profiles.

 

 

Mitchel L. Zoler/Frontline Medical News
Dr. Wenlei Jiang (left) and Dr. Tricia Y. Ting

The third study, BEEP (Bioequivalence in Epilepsy Patients) ran at the University of Maryland, Baltimore, and the results appeared in a journal article published in September (Epilepsia. 2015 Sept;56[9]:1415-24). This study enrolled 34 “generic brittle” epilepsy patients, which meant they had already shown signs of possible sensitivity to switching from Lamictal to generic lamotrigine. The study randomized patients to four consecutive 2-week periods of treatment with either the brand-name or a generic lamotrigine product in a crossover design that was then repeated, and each patient underwent a 12-hour pharmacokinetic analysis after they reached a steady-state drug level with 2 weeks of treatment. The results showed a tight match for both the area under the curve and peak plasma concentration for the generic and brand drugs, said Dr. Tricia Y. Ting, lead investigator for the study and a neurologist and epilepsy specialist at the University of Maryland Medical Center in Baltimore.

“The results could not have been more beautiful. We were quite surprised at how close the generic and brand products were” in their steady-state pharmacokinetic profiles, Dr. Ting said during the session.

The results of the three studies, while reassuring, raise questions as to why some patients nevertheless report problems while taking generic products, noted Dr. Ting. “We need to look outside of bioequivalence, and focus instead on issues such as patient expectations,” she said.

Patient factors

Dr. Joshua J. Gagne, a pharmacoepidemiologist at Brigham and Women’s Hospital in Boston, discussed the role of patient expectations and other patient-specific factors that can affect the safety and efficacy of generic products. He noted that patients can be confused by generic pills that do not have the same size, shape, or color as their brand-name counterparts. “Variations in appearance with generic antiepilepsy drugs is a real problem and may be a barrier to adherence,” he said. In addition, “patients’ out of pocket costs are important drivers of antiepileptic drug adherence,” and may act in favor of generics, he said.

Mitchel L. Zoler/Frontline Medical News
Dr. Joshua J. Gagne

He documented this potential effect in a recent study he published and also summarized while speaking during the session. Dr. Gagne and his associates used a database of more than 19,000 U.S. Medicare patients with epilepsy who began treatment with an antiepileptic drug. The researchers used propensity scoring to match a subset from among the 18,306 patients who started on a generic drug and the 1,454 patients who started on a brand-name drug. In the matched subgroups, those on a generic went an average of 138 days before having a 14-day gap in treatment, compared with an average 124 days until a 14-day treatment gap occurred among those on a branded drug. This difference in adherence linked with a significant difference in seizure-related hospitalizations, experienced by 47 patients who started on a branded drug and in 31 of those who started on a generic. This calculated out to a statistically significant relative risk reduction of more than 50% (Epilepsy Behavior. 2015 Nov;52[part A]:14-8).

Often it is the physician that’s to blame when patients lack trust in a generic drug, noted Dr. Michel J. Berg, a neurologist at the University of Rochester (N.Y.) and coprincipal investigator on the two EQUIGEN studies. “If physicians are confident [in generics] then patients will rely on the physician’s expert opinion,” Dr. Berg said during a panel discussion of these studies during the session.

Patients and physicians also need to realize that today’s generics are often not the same products that they were years ago. The FDA has “encouraged manufacturers to move from ’quality by testing’ to ‘quality by design,’ which has resulted in better products,” stressed Dr. Jiang.

Dr. Privitera agreed. “A lot of the fear about generics was generated 20 or more years ago, when the generic quality was not as good. There were a lot of scary stories out there. Today, with quality by design, manufacturers don’t just try to get their generic in a target range but they do multiple tests earlier in the [generic development] process so that by the time they get to clinical testing they already have a drug that is really tight.”

Members of the audience at the session who commented during the discussion period usually agreed that the new data reported for lamotrigine convinced them of the quality of modern generics. “There has been discomfort with generics, but now we have the data that they are effective and safe,” commented Dr. Mark C. Spitz, professor of neurology and head of the Adult Comprehensive Epilepsy Program at the University of Colorado at Denver, Aurora, who spoke from the floor. “These new data will make a big difference in how epileptologists will practice,” Dr. Spitz predicted.

 

 

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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AES: Three studies show generic lamotrigine equals Lamictal
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Key clinical point: Results from three separate, randomized trials in epilepsy patients showed that generic lamotrigine performed identically to brand-name Lamictal.

Major finding: During chronic treatment, generic lamotrigine produced an area under the curve within 98%-103% of the brand-name, reference product Lamictal.

Data source: The prospective, randomized U.S. trials that respectively enrolled 48, 35, and 34 epilepsy patients.

Disclosures: The two EQUIGEN studies and the BEEP study had no commercial funding. Dr. Jiang had no disclosures. Dr. Privitera has received research funding from UCB, Eisai, and Neuren Pharmaceuticals and has served on the data safety and monitoring boards for trials funded by Astellas and Upsher-Smith. Dr. Ting has received research funding from Acorda and Pfizer. Dr. Gagne has received research funding from Teva and Novartis and is a consultant to Aetion. Dr. Berg has received research funding from Eisai, NeuroPace, Sunovion, Pfizer, Lundbeck, and Acorda. He also is a stockholder in and has patent rights licensed to PharmAdva and Jemsico. Dr. Spitz has been a consultant to Cyberonics.

AES: Many U.S. epilepsy patients receive suboptimal treatment

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AES: Many U.S. epilepsy patients receive suboptimal treatment

PHILADELPHIA – Roughly half of U.S. patients newly diagnosed with epilepsy fail to receive a stable and effective treatment that keeps them seizure free during the first year following their diagnosis, according to an analysis of more than 17,000 incident epilepsy cases who received documented treatment with antiepileptic drugs and had at least 1 year of follow-up.

“Under the best health care circumstances, we can achieve full seizure control in two-thirds to 70% of patients, but the fact that we fall way short points to a treatment gap,” said Dr. David J. Thurman, a neurologist and epilepsy specialist who practices in Atlanta and is affiliated with Emory University. “We’re doing a lousy job,” he said in an interview while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. David J. Thurman

Dr. Thurman suggested that several factors likely contribute to epilepsy patients receiving less than ideal care, including their access to neurologists and epilepsy subspecialists, patients’ ability to afford the drugs they need to control their seizures, and social limitations, such as the ability to travel to see specialists.

He cited a recent study he and his associates published that documented these barriers. They analyzed data collected from U.S. adults in 2010 and 2013 by the National Health Interview Survey run by the Centers for Disease Control and Prevention. That analysis showed that, when compared with the general U.S. adult population, people diagnosed with epilepsy were significantly less likely to be employed and more likely to be disabled. The epilepsy patients also reported relatively higher rates of inability to afford their medications, mental health care, eyeglasses, and dental care, and the patients also reported a relatively high rate of having transportation to health care as a barrier to receiving their care (Epilepsy Behav. 2015 Nov 25. doi: 10.1016/j.yebeh.2015.10.028). CDC data also showed that in 2010, 42% of U.S. adults with epilepsy and uncontrolled seizures had not been seen by a neurologist or epilepsy specialist during the preceding year.

The new report presented by Dr, Thurman at the meeting used U.S. claims data from patients of any age with private insurance or coverage through Medicare or Medicaid contained in the Truven Health Marketscan database during January 2011–June 2013. They identified 36,035 patients who appeared to have newly diagnosed epilepsy, of whom 17,106 received documented treatment for epilepsy during at least 1 year following their diagnosis. About a quarter of these patients had focal epilepsy, about a quarter generalized epilepsy, and about half had undefined epilepsy.

Among these 17,106 patients, 8,835 (52%) appeared to attain “treatment stability,” which the researchers defined as no changes in their antiepileptic drug regimen and no epilepsy-related hospitalizations in either the emergency department or as inpatients. About 42% of the patients reached stability with their first antiepileptic drug, another 6% reached stability with their second drug, and about 3% with their third drug, the researchers reported. The vast majority of patients who attained stability maintained it with monotherapy. Variables that linked with a greater likelihood of achieving treatment stability included older age, male sex, a history of a childhood psychiatric disorder, and having identified focal or generalized epilepsy rather than undefined epilepsy.

The study was funded by UCB. Dr. Thurman has been a consultant to and has received research funding from UCB.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Roughly half of U.S. patients newly diagnosed with epilepsy fail to receive a stable and effective treatment that keeps them seizure free during the first year following their diagnosis, according to an analysis of more than 17,000 incident epilepsy cases who received documented treatment with antiepileptic drugs and had at least 1 year of follow-up.

“Under the best health care circumstances, we can achieve full seizure control in two-thirds to 70% of patients, but the fact that we fall way short points to a treatment gap,” said Dr. David J. Thurman, a neurologist and epilepsy specialist who practices in Atlanta and is affiliated with Emory University. “We’re doing a lousy job,” he said in an interview while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. David J. Thurman

Dr. Thurman suggested that several factors likely contribute to epilepsy patients receiving less than ideal care, including their access to neurologists and epilepsy subspecialists, patients’ ability to afford the drugs they need to control their seizures, and social limitations, such as the ability to travel to see specialists.

He cited a recent study he and his associates published that documented these barriers. They analyzed data collected from U.S. adults in 2010 and 2013 by the National Health Interview Survey run by the Centers for Disease Control and Prevention. That analysis showed that, when compared with the general U.S. adult population, people diagnosed with epilepsy were significantly less likely to be employed and more likely to be disabled. The epilepsy patients also reported relatively higher rates of inability to afford their medications, mental health care, eyeglasses, and dental care, and the patients also reported a relatively high rate of having transportation to health care as a barrier to receiving their care (Epilepsy Behav. 2015 Nov 25. doi: 10.1016/j.yebeh.2015.10.028). CDC data also showed that in 2010, 42% of U.S. adults with epilepsy and uncontrolled seizures had not been seen by a neurologist or epilepsy specialist during the preceding year.

The new report presented by Dr, Thurman at the meeting used U.S. claims data from patients of any age with private insurance or coverage through Medicare or Medicaid contained in the Truven Health Marketscan database during January 2011–June 2013. They identified 36,035 patients who appeared to have newly diagnosed epilepsy, of whom 17,106 received documented treatment for epilepsy during at least 1 year following their diagnosis. About a quarter of these patients had focal epilepsy, about a quarter generalized epilepsy, and about half had undefined epilepsy.

Among these 17,106 patients, 8,835 (52%) appeared to attain “treatment stability,” which the researchers defined as no changes in their antiepileptic drug regimen and no epilepsy-related hospitalizations in either the emergency department or as inpatients. About 42% of the patients reached stability with their first antiepileptic drug, another 6% reached stability with their second drug, and about 3% with their third drug, the researchers reported. The vast majority of patients who attained stability maintained it with monotherapy. Variables that linked with a greater likelihood of achieving treatment stability included older age, male sex, a history of a childhood psychiatric disorder, and having identified focal or generalized epilepsy rather than undefined epilepsy.

The study was funded by UCB. Dr. Thurman has been a consultant to and has received research funding from UCB.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Roughly half of U.S. patients newly diagnosed with epilepsy fail to receive a stable and effective treatment that keeps them seizure free during the first year following their diagnosis, according to an analysis of more than 17,000 incident epilepsy cases who received documented treatment with antiepileptic drugs and had at least 1 year of follow-up.

“Under the best health care circumstances, we can achieve full seizure control in two-thirds to 70% of patients, but the fact that we fall way short points to a treatment gap,” said Dr. David J. Thurman, a neurologist and epilepsy specialist who practices in Atlanta and is affiliated with Emory University. “We’re doing a lousy job,” he said in an interview while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. David J. Thurman

Dr. Thurman suggested that several factors likely contribute to epilepsy patients receiving less than ideal care, including their access to neurologists and epilepsy subspecialists, patients’ ability to afford the drugs they need to control their seizures, and social limitations, such as the ability to travel to see specialists.

He cited a recent study he and his associates published that documented these barriers. They analyzed data collected from U.S. adults in 2010 and 2013 by the National Health Interview Survey run by the Centers for Disease Control and Prevention. That analysis showed that, when compared with the general U.S. adult population, people diagnosed with epilepsy were significantly less likely to be employed and more likely to be disabled. The epilepsy patients also reported relatively higher rates of inability to afford their medications, mental health care, eyeglasses, and dental care, and the patients also reported a relatively high rate of having transportation to health care as a barrier to receiving their care (Epilepsy Behav. 2015 Nov 25. doi: 10.1016/j.yebeh.2015.10.028). CDC data also showed that in 2010, 42% of U.S. adults with epilepsy and uncontrolled seizures had not been seen by a neurologist or epilepsy specialist during the preceding year.

The new report presented by Dr, Thurman at the meeting used U.S. claims data from patients of any age with private insurance or coverage through Medicare or Medicaid contained in the Truven Health Marketscan database during January 2011–June 2013. They identified 36,035 patients who appeared to have newly diagnosed epilepsy, of whom 17,106 received documented treatment for epilepsy during at least 1 year following their diagnosis. About a quarter of these patients had focal epilepsy, about a quarter generalized epilepsy, and about half had undefined epilepsy.

Among these 17,106 patients, 8,835 (52%) appeared to attain “treatment stability,” which the researchers defined as no changes in their antiepileptic drug regimen and no epilepsy-related hospitalizations in either the emergency department or as inpatients. About 42% of the patients reached stability with their first antiepileptic drug, another 6% reached stability with their second drug, and about 3% with their third drug, the researchers reported. The vast majority of patients who attained stability maintained it with monotherapy. Variables that linked with a greater likelihood of achieving treatment stability included older age, male sex, a history of a childhood psychiatric disorder, and having identified focal or generalized epilepsy rather than undefined epilepsy.

The study was funded by UCB. Dr. Thurman has been a consultant to and has received research funding from UCB.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Key clinical point: A sample of newly diagnosed U.S. epilepsy patients showed about half failed to have first-year treatment stability, an indicator that many patients receive suboptimal care.

Major finding: During 2011-2013, about 52% of Americans newly diagnosed with epilepsy achieved treatment “stability.”

Data source: Retrospective review of 17,106 newly diagnosed U.S. epilepsy patients contained in the Truven Health Marketscan database.

Disclosures: The study was funded by UCB. Dr. Thurman has been a consultant to and has received research funding from UCB.

AES: Cannabidiol shows promising epilepsy safety and efficacy

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AES: Cannabidiol shows promising epilepsy safety and efficacy

PHILADELPHIA – A pharmaceutical-grade formulation of orally administered cannabidiol, a cannabis derivative, showed “very positive and promising” safety and efficacy during in an open-label, multicenter, compassionate-use U.S. program that has so far enrolled 313 children and young adults with severe and “extremely” treatment-refractory epilepsy.

In the 261 patients followed on treatment for at least 12 weeks at a total of 16 U.S. centers, patients had a median 49% reduction in their baseline number of monthly convulsant seizures, Dr. Orrin Devinsky said while presenting in a late-breaker poster at the annual meeting of the American Epilepsy Society.

In addition, 47% of these patients had at least a 50% cut in their baseline number of monthly convulsant seizures. And during the final 4 weeks on treatment (weeks 9-12 on treatment), 9% of all patients and 13% of the 44 patients with Dravet syndrome were completely seizure free, reported Dr. Devinsky, professor of neurology and director of the Comprehensive Epilepsy Center at New York University.

Dr. Orrin Devinsky

“In these extremely treatment-refractory patients, these numbers [of seizure-free patients] were much greater than I would have predicted,” Dr. Devinsky said during a press conference. Although he cautioned that a more definitive assessment of the drug’s safety and efficacy will need to await reports of results from four phase III, randomized, placebo-controlled trials that are expected in 2016, “this drug will likely be effective for some patients,” he predicted. “I’m very encouraged by these results.”

The safety analysis, done using data from all 313 patients including those who had not yet received the drug for 12 weeks, showed a “generally well-tolerated” profile, with 4% of patients stopping treatment because of adverse events, 5% experiencing a serious adverse event considered treatment related, and 12% of patients withdrawing because of lack of efficacy.

In a second poster presented at the meeting, investigators at the University of California, San Francisco, one of the other centers involved in this series, reported results for 25 of these patients who they followed on continuous treatment for up to 12 months. In this subgroup, 10 patients (40%) had at least a 50% reduction in their baseline number of convulsant seizures at 12 months, and 1 patient, with Dravet syndrome, was seizure free. During 12 months of follow-up, 12 of the 25 patients discontinued treatment because of lack of efficacy, reported Dr. Michael S. Oldham, a member of the San Francisco group who is now a pediatric neurologist at the University of Louisville (Ky.).

Dr. Michael S. Oldham

Speaking at the same press conference, Dr. Oldham echoed Dr. Devinsky’s assessment of these uncontrolled findings using this cannabidiol formulation. “This was a significantly drug-resistant population, so the fact that we saw at least 50% seizure reductions [in about a third of patients] was remarkable,” he said. “It was exciting to see the results sustained to 12 months with no added adverse events” beyond those seen after 3 months on treatment, Dr. Oldham said in an interview.

Cannabidiol is the most abundant nonpsychoactive cannabinoid contained in cannabis, and the formulation tested in this series contains 99% cannabidiol dissolved in oil. It is being developed by GW Pharmaceuticals under the brand name Epidiolex.

The reported series enrolled patients with various types of juvenile-onset epilepsies, the most common of which was Dravet syndrome. The series also included 40 patients (15%) with Lennox-Gastaut syndrome, and 19% had epilepsy of unknown cause. The enrolled patients averaged 12 years old, ranging from 4 months to 41 years old. At entry enrolled patients averaged 139 convulsant seizures and a median of 31 convulsant seizures every 28 days. The seizure tally focused on convulsant seizures because they are the easiest to reliably identify, Dr. Devinsky noted. The enrolled patients were concurrently on an average of three other antiepileptic drugs. Patients received a gradually escalated dosage until they reached their maximally tolerated dosage or a maximum of 50 mg/kg/day.

The four phase III trials expected to have results reported in 2016 include two that have enrolled patients with Dravet syndrome and two that have enrolled patients with Lennox-Gastaut syndrome. If the tested cannabidiol formulation continues to show good safety and efficacy in those studies and enters the U.S. market, its use will likely gradually expand, first to patients with other severe and drug-refractory forms of epilepsy and then, as experience further grows, to use in less drug-refractory patients, Dr. Devinsky predicted. Both Dr. Devinsky and Dr. Oldham noted that they have heard from several parents who are eager to put their children with milder forms of epilepsy on this formulation, but Dr. Devinsky cautioned that it is much too soon in the drug’s development to consider taking that step.

 

 

Other posters presented at the meeting reported promising efficacy and safety results from small series of pediatric patients with specific, refractory epilepsy syndromes, including 10 children and adolescents with epilepsy in tuberous sclerosis complex, and 9 children and adolescents with refractory epileptic spasms. Both of these studies were run at Massachusetts General Hospital in Boston.

The study received research funding from GW Pharmaceuticals, the company developing the tested formulation of cannabidiol (Epidiolex). Dr. Devinsky and Dr. Oldham had no personal disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – A pharmaceutical-grade formulation of orally administered cannabidiol, a cannabis derivative, showed “very positive and promising” safety and efficacy during in an open-label, multicenter, compassionate-use U.S. program that has so far enrolled 313 children and young adults with severe and “extremely” treatment-refractory epilepsy.

In the 261 patients followed on treatment for at least 12 weeks at a total of 16 U.S. centers, patients had a median 49% reduction in their baseline number of monthly convulsant seizures, Dr. Orrin Devinsky said while presenting in a late-breaker poster at the annual meeting of the American Epilepsy Society.

In addition, 47% of these patients had at least a 50% cut in their baseline number of monthly convulsant seizures. And during the final 4 weeks on treatment (weeks 9-12 on treatment), 9% of all patients and 13% of the 44 patients with Dravet syndrome were completely seizure free, reported Dr. Devinsky, professor of neurology and director of the Comprehensive Epilepsy Center at New York University.

Dr. Orrin Devinsky

“In these extremely treatment-refractory patients, these numbers [of seizure-free patients] were much greater than I would have predicted,” Dr. Devinsky said during a press conference. Although he cautioned that a more definitive assessment of the drug’s safety and efficacy will need to await reports of results from four phase III, randomized, placebo-controlled trials that are expected in 2016, “this drug will likely be effective for some patients,” he predicted. “I’m very encouraged by these results.”

The safety analysis, done using data from all 313 patients including those who had not yet received the drug for 12 weeks, showed a “generally well-tolerated” profile, with 4% of patients stopping treatment because of adverse events, 5% experiencing a serious adverse event considered treatment related, and 12% of patients withdrawing because of lack of efficacy.

In a second poster presented at the meeting, investigators at the University of California, San Francisco, one of the other centers involved in this series, reported results for 25 of these patients who they followed on continuous treatment for up to 12 months. In this subgroup, 10 patients (40%) had at least a 50% reduction in their baseline number of convulsant seizures at 12 months, and 1 patient, with Dravet syndrome, was seizure free. During 12 months of follow-up, 12 of the 25 patients discontinued treatment because of lack of efficacy, reported Dr. Michael S. Oldham, a member of the San Francisco group who is now a pediatric neurologist at the University of Louisville (Ky.).

Dr. Michael S. Oldham

Speaking at the same press conference, Dr. Oldham echoed Dr. Devinsky’s assessment of these uncontrolled findings using this cannabidiol formulation. “This was a significantly drug-resistant population, so the fact that we saw at least 50% seizure reductions [in about a third of patients] was remarkable,” he said. “It was exciting to see the results sustained to 12 months with no added adverse events” beyond those seen after 3 months on treatment, Dr. Oldham said in an interview.

Cannabidiol is the most abundant nonpsychoactive cannabinoid contained in cannabis, and the formulation tested in this series contains 99% cannabidiol dissolved in oil. It is being developed by GW Pharmaceuticals under the brand name Epidiolex.

The reported series enrolled patients with various types of juvenile-onset epilepsies, the most common of which was Dravet syndrome. The series also included 40 patients (15%) with Lennox-Gastaut syndrome, and 19% had epilepsy of unknown cause. The enrolled patients averaged 12 years old, ranging from 4 months to 41 years old. At entry enrolled patients averaged 139 convulsant seizures and a median of 31 convulsant seizures every 28 days. The seizure tally focused on convulsant seizures because they are the easiest to reliably identify, Dr. Devinsky noted. The enrolled patients were concurrently on an average of three other antiepileptic drugs. Patients received a gradually escalated dosage until they reached their maximally tolerated dosage or a maximum of 50 mg/kg/day.

The four phase III trials expected to have results reported in 2016 include two that have enrolled patients with Dravet syndrome and two that have enrolled patients with Lennox-Gastaut syndrome. If the tested cannabidiol formulation continues to show good safety and efficacy in those studies and enters the U.S. market, its use will likely gradually expand, first to patients with other severe and drug-refractory forms of epilepsy and then, as experience further grows, to use in less drug-refractory patients, Dr. Devinsky predicted. Both Dr. Devinsky and Dr. Oldham noted that they have heard from several parents who are eager to put their children with milder forms of epilepsy on this formulation, but Dr. Devinsky cautioned that it is much too soon in the drug’s development to consider taking that step.

 

 

Other posters presented at the meeting reported promising efficacy and safety results from small series of pediatric patients with specific, refractory epilepsy syndromes, including 10 children and adolescents with epilepsy in tuberous sclerosis complex, and 9 children and adolescents with refractory epileptic spasms. Both of these studies were run at Massachusetts General Hospital in Boston.

The study received research funding from GW Pharmaceuticals, the company developing the tested formulation of cannabidiol (Epidiolex). Dr. Devinsky and Dr. Oldham had no personal disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – A pharmaceutical-grade formulation of orally administered cannabidiol, a cannabis derivative, showed “very positive and promising” safety and efficacy during in an open-label, multicenter, compassionate-use U.S. program that has so far enrolled 313 children and young adults with severe and “extremely” treatment-refractory epilepsy.

In the 261 patients followed on treatment for at least 12 weeks at a total of 16 U.S. centers, patients had a median 49% reduction in their baseline number of monthly convulsant seizures, Dr. Orrin Devinsky said while presenting in a late-breaker poster at the annual meeting of the American Epilepsy Society.

In addition, 47% of these patients had at least a 50% cut in their baseline number of monthly convulsant seizures. And during the final 4 weeks on treatment (weeks 9-12 on treatment), 9% of all patients and 13% of the 44 patients with Dravet syndrome were completely seizure free, reported Dr. Devinsky, professor of neurology and director of the Comprehensive Epilepsy Center at New York University.

Dr. Orrin Devinsky

“In these extremely treatment-refractory patients, these numbers [of seizure-free patients] were much greater than I would have predicted,” Dr. Devinsky said during a press conference. Although he cautioned that a more definitive assessment of the drug’s safety and efficacy will need to await reports of results from four phase III, randomized, placebo-controlled trials that are expected in 2016, “this drug will likely be effective for some patients,” he predicted. “I’m very encouraged by these results.”

The safety analysis, done using data from all 313 patients including those who had not yet received the drug for 12 weeks, showed a “generally well-tolerated” profile, with 4% of patients stopping treatment because of adverse events, 5% experiencing a serious adverse event considered treatment related, and 12% of patients withdrawing because of lack of efficacy.

In a second poster presented at the meeting, investigators at the University of California, San Francisco, one of the other centers involved in this series, reported results for 25 of these patients who they followed on continuous treatment for up to 12 months. In this subgroup, 10 patients (40%) had at least a 50% reduction in their baseline number of convulsant seizures at 12 months, and 1 patient, with Dravet syndrome, was seizure free. During 12 months of follow-up, 12 of the 25 patients discontinued treatment because of lack of efficacy, reported Dr. Michael S. Oldham, a member of the San Francisco group who is now a pediatric neurologist at the University of Louisville (Ky.).

Dr. Michael S. Oldham

Speaking at the same press conference, Dr. Oldham echoed Dr. Devinsky’s assessment of these uncontrolled findings using this cannabidiol formulation. “This was a significantly drug-resistant population, so the fact that we saw at least 50% seizure reductions [in about a third of patients] was remarkable,” he said. “It was exciting to see the results sustained to 12 months with no added adverse events” beyond those seen after 3 months on treatment, Dr. Oldham said in an interview.

Cannabidiol is the most abundant nonpsychoactive cannabinoid contained in cannabis, and the formulation tested in this series contains 99% cannabidiol dissolved in oil. It is being developed by GW Pharmaceuticals under the brand name Epidiolex.

The reported series enrolled patients with various types of juvenile-onset epilepsies, the most common of which was Dravet syndrome. The series also included 40 patients (15%) with Lennox-Gastaut syndrome, and 19% had epilepsy of unknown cause. The enrolled patients averaged 12 years old, ranging from 4 months to 41 years old. At entry enrolled patients averaged 139 convulsant seizures and a median of 31 convulsant seizures every 28 days. The seizure tally focused on convulsant seizures because they are the easiest to reliably identify, Dr. Devinsky noted. The enrolled patients were concurrently on an average of three other antiepileptic drugs. Patients received a gradually escalated dosage until they reached their maximally tolerated dosage or a maximum of 50 mg/kg/day.

The four phase III trials expected to have results reported in 2016 include two that have enrolled patients with Dravet syndrome and two that have enrolled patients with Lennox-Gastaut syndrome. If the tested cannabidiol formulation continues to show good safety and efficacy in those studies and enters the U.S. market, its use will likely gradually expand, first to patients with other severe and drug-refractory forms of epilepsy and then, as experience further grows, to use in less drug-refractory patients, Dr. Devinsky predicted. Both Dr. Devinsky and Dr. Oldham noted that they have heard from several parents who are eager to put their children with milder forms of epilepsy on this formulation, but Dr. Devinsky cautioned that it is much too soon in the drug’s development to consider taking that step.

 

 

Other posters presented at the meeting reported promising efficacy and safety results from small series of pediatric patients with specific, refractory epilepsy syndromes, including 10 children and adolescents with epilepsy in tuberous sclerosis complex, and 9 children and adolescents with refractory epileptic spasms. Both of these studies were run at Massachusetts General Hospital in Boston.

The study received research funding from GW Pharmaceuticals, the company developing the tested formulation of cannabidiol (Epidiolex). Dr. Devinsky and Dr. Oldham had no personal disclosures.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Key clinical point: Children and young adults with various severe and treatment-refractory forms of epilepsy who received a pharmaceutical-grade oral cannabidiol formulation showed promising safety and efficacy outcomes during 12 weeks of open-label treatment.

Major finding: After 12 weeks, convulsant seizures dropped from baseline numbers by a median of 49%.

Data source: An open-label series of 313 patients enrolled at any of 16 U.S. centers.

Disclosures: The study received research funding from GW Pharmaceuticals, the company developing the tested formulation of cannabidiol (Epidiolex). Dr. Devinsky and Dr. Oldham had no personal disclosures.

AES: Hormonal contraceptives can boost seizures in epileptics

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PHILADELPHIA – Women with epilepsy often reported having an increased number of seizures when taking a hormonal contraceptive, according to data collected from 1,144 women with epilepsy who completed an online survey.

The data showed that women who used hormonal contraception reported having an increased number of seizures while on the contraceptive about 4.5-fold more often than did women who used nonhormonal contraception. The risk for an increased number of seizures with hormonal contraception seemed greatest for women treated with valproate.

Until now, “valproate was generally accepted as okay to use” by women also taking a hormonal contraceptive, but the new findings suggest that if a woman of childbearing age with epilepsy needs valproate for seizure control she would be better off using a nonhormonal form of contraception such as an intrauterine device, Dr. Andrew G. Herzog said while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. Andrew G. Herzog

Dr. Herzog highlighted the need for some form of contraception for most younger women on valproate because of the drug’s potential teratogenic effects, but he also stressed that the risk for increased seizures does not appear to affect a majority of women. The survey results showed that overall only 28% of women with epilepsy reported an increased seizure frequency when using a hormonal contraceptive.

“The first goal of a neurologist is to get seizures under control, and you go with the [antiepileptic drugs] that work,” Dr. Herzog said in an interview. Once an effective regimen is found, the physician can then deal with other issues, such as adverse effects as well as the potential for an adverse interaction with a hormonal contraceptive. Valproate can be the antiepileptic drug of choice as it is one of the most effective agents for controlling seizures in patients with primary generalized epilepsy, said Dr. Herzog, professor of neurology at Harvard Medical School, Boston, and director of the neuroendocrine unit of Beth Israel Deaconess Medical Center in Wellesley, Mass.

The new data come from an Internet-based survey, which is subject to biases and appeared to attract a preponderance of responses from women who were better educated and had higher incomes than did the general population. In addition, the researchers collected the data retrospectively. Despite these limitations, the results are notable because they represent the only data set yet reported from a community-based source large enough to allow analysis of the many clinical variables that play into the potential interactions between various contraceptive types, various antiepileptic drug classes, and the diverse number of epilepsy subtypes, he said. Dr. Herzog and his associates are planning a study to collect similar data prospectively, but the results would likely not be available for at least about 5 years, he noted.

The Epilepsy Birth Control Registry enrolled women with epilepsy aged 18-47 years who had a history of using at least one form of contraception while on antiepileptic treatment, and the 1,144 women who completed the survey reported a total of 2,712 contraceptive experiences. The survey asked women, “Do you think this method of birth control changed how often you had seizures?” with the option to reply that their contraceptive method seemed to increase, decrease, or not change their seizure number.

One of the analyses done by Dr. Herzog and his associates compared the responses by women on any form of hormonal contraceptive (combined or progestin pill, hormonal patch, vaginal ring, depot medroxyprogesterone acetate, or implanted hormone) with women on any form of nonhormonal contraception (withdrawal, male or female condom, copper or progestin intrauterine device, or tubal ligation).

The results showed that 72% of women on any hormonal contraceptive and 91% of women on any form of nonhormonal contraceptive reported no change in their seizure frequency. The rates of reporting an increased number of seizures were 19% with hormonal contraceptives and 4% with nonhormonal contraceptives, which computed to a relative risk of about 4.5-fold for an increased number of seizures while on hormonal contraception, compared with nonhormonal contraception, the researchers reported.

Barrier contraception (male or female condoms) had the lowest rate of seizure increase among any of the nonhormonal methods. The risk for greater seizure frequency on hormonal contraceptives of all types was 6.75-fold higher when compared specifically with barrier contraception.

In analyses of specific types of hormonal contraceptives, women using a hormonal patch reported a 68% greater incidence of seizure increases, compared with women using combined oral contraceptive pills (the hormonal method that produced the fewest episodes of seizure increases). Those using a progestin-only pill had a 62% higher rate of seizure increases.

 

 

More women on hormonal contraceptives also reported having a decrease in seizures after starting contraception, compared with those starting on a nonhormonal method (9.5% vs. 5.2%, respectively), which calculated to a 85% relative rate increase for decreased seizures. Depot medroxyprogesterone acetate was the only specific hormonal contraceptive that linked with a higher rate of seizure decreases, compared with combined oral pills, a 95% higher rate.

A second analysis of the results by Dr. Herzog and his associates examined the frequencies of seizure outcomes on hormonal and nonhormonal contraceptives stratifying by type of antiepileptic drug women used when starting a particular contraceptive method. This analysis broke down antiepileptic drugs into four types: enzyme inducing (29%), glucuronidated (such as lamotrigine; 27%), nonenzyme inducing (such as levetiracetam; 22%), enzyme inhibiting (valproate; 8%), and a fifth category that included women who were not on any antiepileptic drug (14%).

This analysis showed that the frequency of seizure increases was significantly greater with hormonal contraceptive use, compared with nonhormonal methods, across all five subgroups of antiepileptic drug type. In addition, the frequency of seizure increases with hormonal contraceptives differed significantly, depending on which antiepileptic drug type women used, but these significant differences among the antiepileptic drug types also occurred among women using nonhormonal contraception.

Women receiving a nonenzyme-inducing drug when starting a hormonal contraceptive reported the lowest frequency of seizure increases, a 12% rate. In contrast, women on an enzyme-inhibiting drug, valproate, had the highest rate of increased seizures when starting a hormonal contraceptive, 29%. This calculated out to about a 2.5-fold relative risk increase for having more seizures when starting hormonal contraception while on valproate, compared with women on a nonenzyme-inducing drug, Dr. Herzog reported.

Physicians “need to be on the lookout for the possibility that seizures could increase when women start a hormonal contraceptive,” he concluded.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Women with epilepsy often reported having an increased number of seizures when taking a hormonal contraceptive, according to data collected from 1,144 women with epilepsy who completed an online survey.

The data showed that women who used hormonal contraception reported having an increased number of seizures while on the contraceptive about 4.5-fold more often than did women who used nonhormonal contraception. The risk for an increased number of seizures with hormonal contraception seemed greatest for women treated with valproate.

Until now, “valproate was generally accepted as okay to use” by women also taking a hormonal contraceptive, but the new findings suggest that if a woman of childbearing age with epilepsy needs valproate for seizure control she would be better off using a nonhormonal form of contraception such as an intrauterine device, Dr. Andrew G. Herzog said while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. Andrew G. Herzog

Dr. Herzog highlighted the need for some form of contraception for most younger women on valproate because of the drug’s potential teratogenic effects, but he also stressed that the risk for increased seizures does not appear to affect a majority of women. The survey results showed that overall only 28% of women with epilepsy reported an increased seizure frequency when using a hormonal contraceptive.

“The first goal of a neurologist is to get seizures under control, and you go with the [antiepileptic drugs] that work,” Dr. Herzog said in an interview. Once an effective regimen is found, the physician can then deal with other issues, such as adverse effects as well as the potential for an adverse interaction with a hormonal contraceptive. Valproate can be the antiepileptic drug of choice as it is one of the most effective agents for controlling seizures in patients with primary generalized epilepsy, said Dr. Herzog, professor of neurology at Harvard Medical School, Boston, and director of the neuroendocrine unit of Beth Israel Deaconess Medical Center in Wellesley, Mass.

The new data come from an Internet-based survey, which is subject to biases and appeared to attract a preponderance of responses from women who were better educated and had higher incomes than did the general population. In addition, the researchers collected the data retrospectively. Despite these limitations, the results are notable because they represent the only data set yet reported from a community-based source large enough to allow analysis of the many clinical variables that play into the potential interactions between various contraceptive types, various antiepileptic drug classes, and the diverse number of epilepsy subtypes, he said. Dr. Herzog and his associates are planning a study to collect similar data prospectively, but the results would likely not be available for at least about 5 years, he noted.

The Epilepsy Birth Control Registry enrolled women with epilepsy aged 18-47 years who had a history of using at least one form of contraception while on antiepileptic treatment, and the 1,144 women who completed the survey reported a total of 2,712 contraceptive experiences. The survey asked women, “Do you think this method of birth control changed how often you had seizures?” with the option to reply that their contraceptive method seemed to increase, decrease, or not change their seizure number.

One of the analyses done by Dr. Herzog and his associates compared the responses by women on any form of hormonal contraceptive (combined or progestin pill, hormonal patch, vaginal ring, depot medroxyprogesterone acetate, or implanted hormone) with women on any form of nonhormonal contraception (withdrawal, male or female condom, copper or progestin intrauterine device, or tubal ligation).

The results showed that 72% of women on any hormonal contraceptive and 91% of women on any form of nonhormonal contraceptive reported no change in their seizure frequency. The rates of reporting an increased number of seizures were 19% with hormonal contraceptives and 4% with nonhormonal contraceptives, which computed to a relative risk of about 4.5-fold for an increased number of seizures while on hormonal contraception, compared with nonhormonal contraception, the researchers reported.

Barrier contraception (male or female condoms) had the lowest rate of seizure increase among any of the nonhormonal methods. The risk for greater seizure frequency on hormonal contraceptives of all types was 6.75-fold higher when compared specifically with barrier contraception.

In analyses of specific types of hormonal contraceptives, women using a hormonal patch reported a 68% greater incidence of seizure increases, compared with women using combined oral contraceptive pills (the hormonal method that produced the fewest episodes of seizure increases). Those using a progestin-only pill had a 62% higher rate of seizure increases.

 

 

More women on hormonal contraceptives also reported having a decrease in seizures after starting contraception, compared with those starting on a nonhormonal method (9.5% vs. 5.2%, respectively), which calculated to a 85% relative rate increase for decreased seizures. Depot medroxyprogesterone acetate was the only specific hormonal contraceptive that linked with a higher rate of seizure decreases, compared with combined oral pills, a 95% higher rate.

A second analysis of the results by Dr. Herzog and his associates examined the frequencies of seizure outcomes on hormonal and nonhormonal contraceptives stratifying by type of antiepileptic drug women used when starting a particular contraceptive method. This analysis broke down antiepileptic drugs into four types: enzyme inducing (29%), glucuronidated (such as lamotrigine; 27%), nonenzyme inducing (such as levetiracetam; 22%), enzyme inhibiting (valproate; 8%), and a fifth category that included women who were not on any antiepileptic drug (14%).

This analysis showed that the frequency of seizure increases was significantly greater with hormonal contraceptive use, compared with nonhormonal methods, across all five subgroups of antiepileptic drug type. In addition, the frequency of seizure increases with hormonal contraceptives differed significantly, depending on which antiepileptic drug type women used, but these significant differences among the antiepileptic drug types also occurred among women using nonhormonal contraception.

Women receiving a nonenzyme-inducing drug when starting a hormonal contraceptive reported the lowest frequency of seizure increases, a 12% rate. In contrast, women on an enzyme-inhibiting drug, valproate, had the highest rate of increased seizures when starting a hormonal contraceptive, 29%. This calculated out to about a 2.5-fold relative risk increase for having more seizures when starting hormonal contraception while on valproate, compared with women on a nonenzyme-inducing drug, Dr. Herzog reported.

Physicians “need to be on the lookout for the possibility that seizures could increase when women start a hormonal contraceptive,” he concluded.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Women with epilepsy often reported having an increased number of seizures when taking a hormonal contraceptive, according to data collected from 1,144 women with epilepsy who completed an online survey.

The data showed that women who used hormonal contraception reported having an increased number of seizures while on the contraceptive about 4.5-fold more often than did women who used nonhormonal contraception. The risk for an increased number of seizures with hormonal contraception seemed greatest for women treated with valproate.

Until now, “valproate was generally accepted as okay to use” by women also taking a hormonal contraceptive, but the new findings suggest that if a woman of childbearing age with epilepsy needs valproate for seizure control she would be better off using a nonhormonal form of contraception such as an intrauterine device, Dr. Andrew G. Herzog said while presenting a poster at the annual meeting of the American Epilepsy Society.

Dr. Andrew G. Herzog

Dr. Herzog highlighted the need for some form of contraception for most younger women on valproate because of the drug’s potential teratogenic effects, but he also stressed that the risk for increased seizures does not appear to affect a majority of women. The survey results showed that overall only 28% of women with epilepsy reported an increased seizure frequency when using a hormonal contraceptive.

“The first goal of a neurologist is to get seizures under control, and you go with the [antiepileptic drugs] that work,” Dr. Herzog said in an interview. Once an effective regimen is found, the physician can then deal with other issues, such as adverse effects as well as the potential for an adverse interaction with a hormonal contraceptive. Valproate can be the antiepileptic drug of choice as it is one of the most effective agents for controlling seizures in patients with primary generalized epilepsy, said Dr. Herzog, professor of neurology at Harvard Medical School, Boston, and director of the neuroendocrine unit of Beth Israel Deaconess Medical Center in Wellesley, Mass.

The new data come from an Internet-based survey, which is subject to biases and appeared to attract a preponderance of responses from women who were better educated and had higher incomes than did the general population. In addition, the researchers collected the data retrospectively. Despite these limitations, the results are notable because they represent the only data set yet reported from a community-based source large enough to allow analysis of the many clinical variables that play into the potential interactions between various contraceptive types, various antiepileptic drug classes, and the diverse number of epilepsy subtypes, he said. Dr. Herzog and his associates are planning a study to collect similar data prospectively, but the results would likely not be available for at least about 5 years, he noted.

The Epilepsy Birth Control Registry enrolled women with epilepsy aged 18-47 years who had a history of using at least one form of contraception while on antiepileptic treatment, and the 1,144 women who completed the survey reported a total of 2,712 contraceptive experiences. The survey asked women, “Do you think this method of birth control changed how often you had seizures?” with the option to reply that their contraceptive method seemed to increase, decrease, or not change their seizure number.

One of the analyses done by Dr. Herzog and his associates compared the responses by women on any form of hormonal contraceptive (combined or progestin pill, hormonal patch, vaginal ring, depot medroxyprogesterone acetate, or implanted hormone) with women on any form of nonhormonal contraception (withdrawal, male or female condom, copper or progestin intrauterine device, or tubal ligation).

The results showed that 72% of women on any hormonal contraceptive and 91% of women on any form of nonhormonal contraceptive reported no change in their seizure frequency. The rates of reporting an increased number of seizures were 19% with hormonal contraceptives and 4% with nonhormonal contraceptives, which computed to a relative risk of about 4.5-fold for an increased number of seizures while on hormonal contraception, compared with nonhormonal contraception, the researchers reported.

Barrier contraception (male or female condoms) had the lowest rate of seizure increase among any of the nonhormonal methods. The risk for greater seizure frequency on hormonal contraceptives of all types was 6.75-fold higher when compared specifically with barrier contraception.

In analyses of specific types of hormonal contraceptives, women using a hormonal patch reported a 68% greater incidence of seizure increases, compared with women using combined oral contraceptive pills (the hormonal method that produced the fewest episodes of seizure increases). Those using a progestin-only pill had a 62% higher rate of seizure increases.

 

 

More women on hormonal contraceptives also reported having a decrease in seizures after starting contraception, compared with those starting on a nonhormonal method (9.5% vs. 5.2%, respectively), which calculated to a 85% relative rate increase for decreased seizures. Depot medroxyprogesterone acetate was the only specific hormonal contraceptive that linked with a higher rate of seizure decreases, compared with combined oral pills, a 95% higher rate.

A second analysis of the results by Dr. Herzog and his associates examined the frequencies of seizure outcomes on hormonal and nonhormonal contraceptives stratifying by type of antiepileptic drug women used when starting a particular contraceptive method. This analysis broke down antiepileptic drugs into four types: enzyme inducing (29%), glucuronidated (such as lamotrigine; 27%), nonenzyme inducing (such as levetiracetam; 22%), enzyme inhibiting (valproate; 8%), and a fifth category that included women who were not on any antiepileptic drug (14%).

This analysis showed that the frequency of seizure increases was significantly greater with hormonal contraceptive use, compared with nonhormonal methods, across all five subgroups of antiepileptic drug type. In addition, the frequency of seizure increases with hormonal contraceptives differed significantly, depending on which antiepileptic drug type women used, but these significant differences among the antiepileptic drug types also occurred among women using nonhormonal contraception.

Women receiving a nonenzyme-inducing drug when starting a hormonal contraceptive reported the lowest frequency of seizure increases, a 12% rate. In contrast, women on an enzyme-inhibiting drug, valproate, had the highest rate of increased seizures when starting a hormonal contraceptive, 29%. This calculated out to about a 2.5-fold relative risk increase for having more seizures when starting hormonal contraception while on valproate, compared with women on a nonenzyme-inducing drug, Dr. Herzog reported.

Physicians “need to be on the lookout for the possibility that seizures could increase when women start a hormonal contraceptive,” he concluded.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Key clinical point: Women with epilepsy often reported having more seizures while taking a hormonal contraceptive, compared with women using nonhormonal contraception.

Major finding: Epileptic women reported a 4.5-fold higher rate of increased seizures when using hormonal contraception, compared with nonhormonal contraception.

Data source: Internet-based survey completed by 1,144 women with epilepsy.

Disclosures: The study received partial support from Lundbeck. Dr. Herzog had no personal disclosures.

AES: Neurologists ignore low driving risk from epilepsy-drug withdrawal

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AES: Neurologists ignore low driving risk from epilepsy-drug withdrawal

PHILADELPHIA – Many U.S. epilepsy specialists take a conservative stance and advise their patients not to drive when they have been seizure free for more than 2 years and taper off of anti-seizure medications or have just stopped medications altogether, based on survey replies from more than 400 U.S. neurologists.

Roughly two-thirds of these physicians said they advise their tapering-down epilepsy patients not to drive even though these patients face about a 0.3% annual risk for a seizure while driving if they drive for 30 minutes a day, Dr. Joon-Yi Kang said in a poster she presented at the annual meeting of the American Epilepsy Society. And more than half the surveyed neurologists advised abstaining from all driving during the 3-6 months after taper down completes and patients are completely off anti-seizure therapy.

Dr. Joon-Yi Kang

Neurologists who advise their epilepsy patients who are tapering down or recently stopped anti-seizure medications “need to think more carefully” about the actual risk patients face when driving, suggested Dr. Kang, a neurologist at Johns Hopkins Hospital in Baltimore. Typically neurologists advise patients to taper down medications after they have been seizure free for at least 2 years, she said in an interview. No U.S. guidelines cover driving once seizure-free epilepsy patients start to withdraw from treatment and no states have laws that cover this situation, she noted.

Once tapering-down of treatment begins, the immediate risk for a seizure runs from 12%-30%, based on published reports, with the risk dropping below 20% once a patient has been seizure free for at least 3 months on gradually reduced treatment or completely stopped treatment, she noted. Based on this Dr. Kang estimated that during the first year of taper down and then full withdrawal the average U.S. epilepsy patient has an overall seizure risk of 15%. If this patient drove 30 minutes each day their average seizure rate while driving would be about 0.3% for the entire year, she reported in her poster.

“This sort of calculation is usually not done” but estimating the risk faced by each patient and discussing that risk with each patient is important, she said. “Some patients stay on their medications just so that they can continue to drive. We need to carefully think about what is an acceptable level of risk.” The restrictions many neurologists recommend to patients “unnecessarily limit patient function,” Dr. Kang said.

She and her co-author sent their survey to 2,028 neurologist members of the American Epilepsy Society and received replies from 411 (20%) in 42 states. About 80% of respondents said that more than half of their practice involved patients with epilepsy, and about 70% said that they had at least 5 years of clinical experience.

During the taper-down period, 65% of respondents said they advise patients to not drive and an additional 24% said they advise patients to minimize their driving. Once patients totally withdrew from treatment, 53% advised continuing to restrict all driving, usually for an additional 3-6 months, and 26% said they advise patients to minimize driving. In addition, 89% of respondents said that their recommendations to restrict or minimize driving often prompted patients to remain on treatment. “I think these findings reflect usual practice” among U.S. neurologists, Dr. Kang said.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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PHILADELPHIA – Many U.S. epilepsy specialists take a conservative stance and advise their patients not to drive when they have been seizure free for more than 2 years and taper off of anti-seizure medications or have just stopped medications altogether, based on survey replies from more than 400 U.S. neurologists.

Roughly two-thirds of these physicians said they advise their tapering-down epilepsy patients not to drive even though these patients face about a 0.3% annual risk for a seizure while driving if they drive for 30 minutes a day, Dr. Joon-Yi Kang said in a poster she presented at the annual meeting of the American Epilepsy Society. And more than half the surveyed neurologists advised abstaining from all driving during the 3-6 months after taper down completes and patients are completely off anti-seizure therapy.

Dr. Joon-Yi Kang

Neurologists who advise their epilepsy patients who are tapering down or recently stopped anti-seizure medications “need to think more carefully” about the actual risk patients face when driving, suggested Dr. Kang, a neurologist at Johns Hopkins Hospital in Baltimore. Typically neurologists advise patients to taper down medications after they have been seizure free for at least 2 years, she said in an interview. No U.S. guidelines cover driving once seizure-free epilepsy patients start to withdraw from treatment and no states have laws that cover this situation, she noted.

Once tapering-down of treatment begins, the immediate risk for a seizure runs from 12%-30%, based on published reports, with the risk dropping below 20% once a patient has been seizure free for at least 3 months on gradually reduced treatment or completely stopped treatment, she noted. Based on this Dr. Kang estimated that during the first year of taper down and then full withdrawal the average U.S. epilepsy patient has an overall seizure risk of 15%. If this patient drove 30 minutes each day their average seizure rate while driving would be about 0.3% for the entire year, she reported in her poster.

“This sort of calculation is usually not done” but estimating the risk faced by each patient and discussing that risk with each patient is important, she said. “Some patients stay on their medications just so that they can continue to drive. We need to carefully think about what is an acceptable level of risk.” The restrictions many neurologists recommend to patients “unnecessarily limit patient function,” Dr. Kang said.

She and her co-author sent their survey to 2,028 neurologist members of the American Epilepsy Society and received replies from 411 (20%) in 42 states. About 80% of respondents said that more than half of their practice involved patients with epilepsy, and about 70% said that they had at least 5 years of clinical experience.

During the taper-down period, 65% of respondents said they advise patients to not drive and an additional 24% said they advise patients to minimize their driving. Once patients totally withdrew from treatment, 53% advised continuing to restrict all driving, usually for an additional 3-6 months, and 26% said they advise patients to minimize driving. In addition, 89% of respondents said that their recommendations to restrict or minimize driving often prompted patients to remain on treatment. “I think these findings reflect usual practice” among U.S. neurologists, Dr. Kang said.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

PHILADELPHIA – Many U.S. epilepsy specialists take a conservative stance and advise their patients not to drive when they have been seizure free for more than 2 years and taper off of anti-seizure medications or have just stopped medications altogether, based on survey replies from more than 400 U.S. neurologists.

Roughly two-thirds of these physicians said they advise their tapering-down epilepsy patients not to drive even though these patients face about a 0.3% annual risk for a seizure while driving if they drive for 30 minutes a day, Dr. Joon-Yi Kang said in a poster she presented at the annual meeting of the American Epilepsy Society. And more than half the surveyed neurologists advised abstaining from all driving during the 3-6 months after taper down completes and patients are completely off anti-seizure therapy.

Dr. Joon-Yi Kang

Neurologists who advise their epilepsy patients who are tapering down or recently stopped anti-seizure medications “need to think more carefully” about the actual risk patients face when driving, suggested Dr. Kang, a neurologist at Johns Hopkins Hospital in Baltimore. Typically neurologists advise patients to taper down medications after they have been seizure free for at least 2 years, she said in an interview. No U.S. guidelines cover driving once seizure-free epilepsy patients start to withdraw from treatment and no states have laws that cover this situation, she noted.

Once tapering-down of treatment begins, the immediate risk for a seizure runs from 12%-30%, based on published reports, with the risk dropping below 20% once a patient has been seizure free for at least 3 months on gradually reduced treatment or completely stopped treatment, she noted. Based on this Dr. Kang estimated that during the first year of taper down and then full withdrawal the average U.S. epilepsy patient has an overall seizure risk of 15%. If this patient drove 30 minutes each day their average seizure rate while driving would be about 0.3% for the entire year, she reported in her poster.

“This sort of calculation is usually not done” but estimating the risk faced by each patient and discussing that risk with each patient is important, she said. “Some patients stay on their medications just so that they can continue to drive. We need to carefully think about what is an acceptable level of risk.” The restrictions many neurologists recommend to patients “unnecessarily limit patient function,” Dr. Kang said.

She and her co-author sent their survey to 2,028 neurologist members of the American Epilepsy Society and received replies from 411 (20%) in 42 states. About 80% of respondents said that more than half of their practice involved patients with epilepsy, and about 70% said that they had at least 5 years of clinical experience.

During the taper-down period, 65% of respondents said they advise patients to not drive and an additional 24% said they advise patients to minimize their driving. Once patients totally withdrew from treatment, 53% advised continuing to restrict all driving, usually for an additional 3-6 months, and 26% said they advise patients to minimize driving. In addition, 89% of respondents said that their recommendations to restrict or minimize driving often prompted patients to remain on treatment. “I think these findings reflect usual practice” among U.S. neurologists, Dr. Kang said.

mzoler@frontlinemedcom.com

On Twitter @mitchelzoler

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Key clinical point: Although epilepsy patients tapering off anti-seizure medication face a less than 1% seizure risk when driving neurologists usually advise them not to drive.

Major finding: Nearly two-thirds of surveyed U.S. neurologists advised patients withdrawing from anti-seizure medications not to drive.

Data source: Survey responses from 411 U.S. neurologists who specialize in epilepsy treatment.

Disclosures: Dr. Kang had no disclosures.