What are effective treatments for panic disorder?

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EVIDENCE-BASED ANSWER

Selective serotonin reuptake inhibitors (SSRIs), tricyclic antidepressants (TCAs), benzodiazepines (BDZs), and cognitive behavioral therapy (CBT) are effective for panic disorder (PD) with or without agoraphobia (NNT5 for complete remission). SSRIs may be most effective, but BDZs work faster. Clomipramine is more effective than other TCAs. CBT improves response and decreases relapse rates when used with medication. Severe symptoms may warrant short-term use of a BDZ until other therapies take effect (Grade of recommendation: A, based on systematic reviews of randomized clinical trials (RCTs); high quality RCTs).

 

Evidence summary

SSRIs were more effective than imipramine or alprazolam in a meta-analysis,1 but equivalent to these drugs in an effect-size analysis.2 The absolute difference in efficacy is difficult to determine; few studies directly compare SSRIs with other drugs. In 2 randomized head-to-head trials,3,4 remission rates (eliminating symptoms) were 50%-65% for paroxetine, 37%-53% for clomipramine, and 32%-34% for placebo after 9-12 weeks of therapy; differences between the 2 active drugs were not significant. Clomipramine is serotoninergic and was more effective than other tricyclics in an RCT.5 Adding a BDZ to an SSRI for the first 3 weeks can rapidly stabilize symptoms6 (Table).

Two meta-analyses concluded that CBT is as effective as antidepressants or BDZs during acute treatment7 and during long-term follow-up (31-121 weeks).8 CBT and imipramine each reduce symptoms in 45%-48% of patients; combining them reduces symptoms in 60%.9 Imipramine is more effective initially; CBT is more durable9 but effects may be therapist-dependent. When used in conjunction with medication, graded exposure to panicinducing situations reduces agoraphobia7 but does not improve relapse rates.8 Behavioral therapy with exposure homework has good long-term results.10

An adequate trial of medication requires 6-8 weeks.11 Before treating, evaluate patients for comorbid mood, anxiety, personality, substance use, or medical disorders, which affect 40%-50% of patients with panic disorder, and may influence the choice of treatment.12 Current practice is to slowly taper and discontinue medication after 12-18 months of maintenance treatment12 if there are no significant residual symptoms, no increased psychosocial stressors, and no history of severe or recurrent relapse.

TABLE
Drugs used to treat panic disorder

Drug ClassSide EffectsOther Considerations
Selective serotonin reuptake inhibitorsNausea (10-30%), drowsiness (7-20%), insomnia (< 10%), nervousness(< 10%), sexual dysfunction (< 10% but underreported).All equivalently effective. Some patients may respond to lower than usual doses. Start at half the usual dose.
Tricyclic antidepressantsDry mouth (> 45%), dizziness (2%), constipation (15%), sweating (15%), tremors (15%), fatigue (< 10%)Requires more time to titrate to treatment dose. Clomipramine more effective. Some patients with panic disorder are extremely sensitive both to the therapeutic and adverse effects of TCAs. Start at very low doses.
BenzodiazepinesSomnolence (15-34%) and impaired coordination (6-22%). Potential for physical dependence and withdrawal symptoms, but psychological addiction has not been a significant problem in clinical trials.Faster onset of action than antidepressants, but do not treat comorbid depression and are more difficult to discontinue.

Recommendations from others

The American Psychiatric Association Guideline states that CBT and pharmacotherapy are equivalently effective, and that SSRIs, TCAs, BDZs, and MAOIs are equivalently effective.12 The International Consensus Group on Depression and Anxiety concludes that SSRIs, TCAs, and BDZs are effective. SSRIs and BDZs are tolerated better than TCAs, and BDZs act faster (1 week vs. 4-8 weeks).11

Read a Clinical Commentary by William A. Hensel, MD, at www.fpin.org.

References

1. Boyer W. Int Clin Psychopharmacol 1995;10:45-9.

2. Otto MW, Tuby KS, Gould RA, et al. Am J Psychiatry 2001;158:1989-92.

3. Lecrubier Y, Bakker A, Dunbar G, et al. Acta Psychiatrica Scand 1997;95:145-52.

4. Bakker A, van Dyck R, Spinhoven P, et al. J Clin Psychiatry 1999;60:831-8.

5. Modigh K, Westberg P, Eriksson E. J Clin Psychopharmacol 1992;12:251-61.

6. Goddard AW, Brouette T, Almai A, et al. Arch Gen Psychiatry 2001;58:681-6.

7. van Balkom A, Bakker A, Spinhoven P, et al. J Nerv Ment Dis 1997;185:510-6.

8. Bakker A, van Balkom A, Spinhoven P, et al. J Nerv Ment Dis 1998;186:414-9.

9. Barlow D, Gorman J, Shear M, et al. JAMA 2000;283:2529-36.

10. Fava GA, Rafanelli C, Grandi S, et al. Psychol Med 2001;31(5):891-8.

11. Ballenger J, Davidson J, Lecrubier Y, et al. J Clin Psychiatry 1998;59(suppl 8):47-54.

12. American Psychiatric Association. Am J Psychiatry 1998;155(5 Suppl):1S-34S.

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EVIDENCE-BASED ANSWER

Selective serotonin reuptake inhibitors (SSRIs), tricyclic antidepressants (TCAs), benzodiazepines (BDZs), and cognitive behavioral therapy (CBT) are effective for panic disorder (PD) with or without agoraphobia (NNT5 for complete remission). SSRIs may be most effective, but BDZs work faster. Clomipramine is more effective than other TCAs. CBT improves response and decreases relapse rates when used with medication. Severe symptoms may warrant short-term use of a BDZ until other therapies take effect (Grade of recommendation: A, based on systematic reviews of randomized clinical trials (RCTs); high quality RCTs).

 

Evidence summary

SSRIs were more effective than imipramine or alprazolam in a meta-analysis,1 but equivalent to these drugs in an effect-size analysis.2 The absolute difference in efficacy is difficult to determine; few studies directly compare SSRIs with other drugs. In 2 randomized head-to-head trials,3,4 remission rates (eliminating symptoms) were 50%-65% for paroxetine, 37%-53% for clomipramine, and 32%-34% for placebo after 9-12 weeks of therapy; differences between the 2 active drugs were not significant. Clomipramine is serotoninergic and was more effective than other tricyclics in an RCT.5 Adding a BDZ to an SSRI for the first 3 weeks can rapidly stabilize symptoms6 (Table).

Two meta-analyses concluded that CBT is as effective as antidepressants or BDZs during acute treatment7 and during long-term follow-up (31-121 weeks).8 CBT and imipramine each reduce symptoms in 45%-48% of patients; combining them reduces symptoms in 60%.9 Imipramine is more effective initially; CBT is more durable9 but effects may be therapist-dependent. When used in conjunction with medication, graded exposure to panicinducing situations reduces agoraphobia7 but does not improve relapse rates.8 Behavioral therapy with exposure homework has good long-term results.10

An adequate trial of medication requires 6-8 weeks.11 Before treating, evaluate patients for comorbid mood, anxiety, personality, substance use, or medical disorders, which affect 40%-50% of patients with panic disorder, and may influence the choice of treatment.12 Current practice is to slowly taper and discontinue medication after 12-18 months of maintenance treatment12 if there are no significant residual symptoms, no increased psychosocial stressors, and no history of severe or recurrent relapse.

TABLE
Drugs used to treat panic disorder

Drug ClassSide EffectsOther Considerations
Selective serotonin reuptake inhibitorsNausea (10-30%), drowsiness (7-20%), insomnia (< 10%), nervousness(< 10%), sexual dysfunction (< 10% but underreported).All equivalently effective. Some patients may respond to lower than usual doses. Start at half the usual dose.
Tricyclic antidepressantsDry mouth (> 45%), dizziness (2%), constipation (15%), sweating (15%), tremors (15%), fatigue (< 10%)Requires more time to titrate to treatment dose. Clomipramine more effective. Some patients with panic disorder are extremely sensitive both to the therapeutic and adverse effects of TCAs. Start at very low doses.
BenzodiazepinesSomnolence (15-34%) and impaired coordination (6-22%). Potential for physical dependence and withdrawal symptoms, but psychological addiction has not been a significant problem in clinical trials.Faster onset of action than antidepressants, but do not treat comorbid depression and are more difficult to discontinue.

Recommendations from others

The American Psychiatric Association Guideline states that CBT and pharmacotherapy are equivalently effective, and that SSRIs, TCAs, BDZs, and MAOIs are equivalently effective.12 The International Consensus Group on Depression and Anxiety concludes that SSRIs, TCAs, and BDZs are effective. SSRIs and BDZs are tolerated better than TCAs, and BDZs act faster (1 week vs. 4-8 weeks).11

Read a Clinical Commentary by William A. Hensel, MD, at www.fpin.org.

EVIDENCE-BASED ANSWER

Selective serotonin reuptake inhibitors (SSRIs), tricyclic antidepressants (TCAs), benzodiazepines (BDZs), and cognitive behavioral therapy (CBT) are effective for panic disorder (PD) with or without agoraphobia (NNT5 for complete remission). SSRIs may be most effective, but BDZs work faster. Clomipramine is more effective than other TCAs. CBT improves response and decreases relapse rates when used with medication. Severe symptoms may warrant short-term use of a BDZ until other therapies take effect (Grade of recommendation: A, based on systematic reviews of randomized clinical trials (RCTs); high quality RCTs).

 

Evidence summary

SSRIs were more effective than imipramine or alprazolam in a meta-analysis,1 but equivalent to these drugs in an effect-size analysis.2 The absolute difference in efficacy is difficult to determine; few studies directly compare SSRIs with other drugs. In 2 randomized head-to-head trials,3,4 remission rates (eliminating symptoms) were 50%-65% for paroxetine, 37%-53% for clomipramine, and 32%-34% for placebo after 9-12 weeks of therapy; differences between the 2 active drugs were not significant. Clomipramine is serotoninergic and was more effective than other tricyclics in an RCT.5 Adding a BDZ to an SSRI for the first 3 weeks can rapidly stabilize symptoms6 (Table).

Two meta-analyses concluded that CBT is as effective as antidepressants or BDZs during acute treatment7 and during long-term follow-up (31-121 weeks).8 CBT and imipramine each reduce symptoms in 45%-48% of patients; combining them reduces symptoms in 60%.9 Imipramine is more effective initially; CBT is more durable9 but effects may be therapist-dependent. When used in conjunction with medication, graded exposure to panicinducing situations reduces agoraphobia7 but does not improve relapse rates.8 Behavioral therapy with exposure homework has good long-term results.10

An adequate trial of medication requires 6-8 weeks.11 Before treating, evaluate patients for comorbid mood, anxiety, personality, substance use, or medical disorders, which affect 40%-50% of patients with panic disorder, and may influence the choice of treatment.12 Current practice is to slowly taper and discontinue medication after 12-18 months of maintenance treatment12 if there are no significant residual symptoms, no increased psychosocial stressors, and no history of severe or recurrent relapse.

TABLE
Drugs used to treat panic disorder

Drug ClassSide EffectsOther Considerations
Selective serotonin reuptake inhibitorsNausea (10-30%), drowsiness (7-20%), insomnia (< 10%), nervousness(< 10%), sexual dysfunction (< 10% but underreported).All equivalently effective. Some patients may respond to lower than usual doses. Start at half the usual dose.
Tricyclic antidepressantsDry mouth (> 45%), dizziness (2%), constipation (15%), sweating (15%), tremors (15%), fatigue (< 10%)Requires more time to titrate to treatment dose. Clomipramine more effective. Some patients with panic disorder are extremely sensitive both to the therapeutic and adverse effects of TCAs. Start at very low doses.
BenzodiazepinesSomnolence (15-34%) and impaired coordination (6-22%). Potential for physical dependence and withdrawal symptoms, but psychological addiction has not been a significant problem in clinical trials.Faster onset of action than antidepressants, but do not treat comorbid depression and are more difficult to discontinue.

Recommendations from others

The American Psychiatric Association Guideline states that CBT and pharmacotherapy are equivalently effective, and that SSRIs, TCAs, BDZs, and MAOIs are equivalently effective.12 The International Consensus Group on Depression and Anxiety concludes that SSRIs, TCAs, and BDZs are effective. SSRIs and BDZs are tolerated better than TCAs, and BDZs act faster (1 week vs. 4-8 weeks).11

Read a Clinical Commentary by William A. Hensel, MD, at www.fpin.org.

References

1. Boyer W. Int Clin Psychopharmacol 1995;10:45-9.

2. Otto MW, Tuby KS, Gould RA, et al. Am J Psychiatry 2001;158:1989-92.

3. Lecrubier Y, Bakker A, Dunbar G, et al. Acta Psychiatrica Scand 1997;95:145-52.

4. Bakker A, van Dyck R, Spinhoven P, et al. J Clin Psychiatry 1999;60:831-8.

5. Modigh K, Westberg P, Eriksson E. J Clin Psychopharmacol 1992;12:251-61.

6. Goddard AW, Brouette T, Almai A, et al. Arch Gen Psychiatry 2001;58:681-6.

7. van Balkom A, Bakker A, Spinhoven P, et al. J Nerv Ment Dis 1997;185:510-6.

8. Bakker A, van Balkom A, Spinhoven P, et al. J Nerv Ment Dis 1998;186:414-9.

9. Barlow D, Gorman J, Shear M, et al. JAMA 2000;283:2529-36.

10. Fava GA, Rafanelli C, Grandi S, et al. Psychol Med 2001;31(5):891-8.

11. Ballenger J, Davidson J, Lecrubier Y, et al. J Clin Psychiatry 1998;59(suppl 8):47-54.

12. American Psychiatric Association. Am J Psychiatry 1998;155(5 Suppl):1S-34S.

References

1. Boyer W. Int Clin Psychopharmacol 1995;10:45-9.

2. Otto MW, Tuby KS, Gould RA, et al. Am J Psychiatry 2001;158:1989-92.

3. Lecrubier Y, Bakker A, Dunbar G, et al. Acta Psychiatrica Scand 1997;95:145-52.

4. Bakker A, van Dyck R, Spinhoven P, et al. J Clin Psychiatry 1999;60:831-8.

5. Modigh K, Westberg P, Eriksson E. J Clin Psychopharmacol 1992;12:251-61.

6. Goddard AW, Brouette T, Almai A, et al. Arch Gen Psychiatry 2001;58:681-6.

7. van Balkom A, Bakker A, Spinhoven P, et al. J Nerv Ment Dis 1997;185:510-6.

8. Bakker A, van Balkom A, Spinhoven P, et al. J Nerv Ment Dis 1998;186:414-9.

9. Barlow D, Gorman J, Shear M, et al. JAMA 2000;283:2529-36.

10. Fava GA, Rafanelli C, Grandi S, et al. Psychol Med 2001;31(5):891-8.

11. Ballenger J, Davidson J, Lecrubier Y, et al. J Clin Psychiatry 1998;59(suppl 8):47-54.

12. American Psychiatric Association. Am J Psychiatry 1998;155(5 Suppl):1S-34S.

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To Screen or Not to Screen? Bacterial Vaginosis in Pregnancy

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To Screen or Not to Screen? Bacterial Vaginosis in Pregnancy

Bacterial vaginosis (BV) is a common condition in which the normal vaginal microflora are replaced by a polymicrobial overgrowth that includes Gardnerella vaginalis, Mycoplasma hominis, and anaerobes such as nonfragilis bacteroides, Mobiluncus, and peptococcus.1 It is now clear that bacterial vaginosis is associated with an increased risk of preterm delivery. The meta-analysis by Flynn and colleagues2 shows that the odds ratio of preterm delivery for patients with bacterial vaginosis during pregnancy is approximately 1.6. Although this is not an enormous increase in risk, it is both statistically and clinically significant. However, the association between BV and preterm delivery does not prove causation or that prenatal screening and treatment will improve perinatal outcomes.

Flynn and coworkers have carried out a detailed and thoughtful meta-analysis, but even a meta-analysis cannot overcome the inherent biases of the underlying case control and cohort studies which can not prove cause and effect. The Heart and Estrogen/Progestin Replacement Study3 demonstrated this phenomenon. That randomized placebo-controlled trial of postmenopausal hormone replacement therapy did not show the reduction in cardiac events that had been expected on the basis of previous observational case control and cohort data.

In the context of preterm delivery, BV is undoubtedly only a marker for something else—presumably subclinical infection of the upper genital tract—which then leads to preterm delivery. The combination of microbes that causes the upper tract infection is not known for certain. Studies in which the authors attempted to treat BV during pregnancy have shown no improvement in perinatal outcomes with oral amoxicillin4 or topical vaginal clindamycin,5,6 supporting the theory that anaerobic infection of the upper genital tract is the link between BV and preterm delivery. Spontaneous regression of BV during pregnancy assessed by vaginal gram stain also does not appear to improve perinatal outcomes, which again supports the idea that BV is not the direct cause of preterm delivery.

Three studies have shown that prenatal screening and treatment with oral metronidazole or with metronidazole and erythromycin seems to reduce the incidence of preterm delivery in patients with BV who also have other risk factors, such as a history of a previous preterm delivery or a low prepregnancy weight.8-10 However, 2 of these studies were weakened by methodologic problems8,10 or small sample numbers.10 These results need to be replicated in larger studies of high-risk women before they can be considered reliable. The case for screening and treating low-risk women is even less clear.

If BV is a marker for something else, would treating all high-risk women, even those without BV, also reduce the number of preterm deliveries? Hauth and colleagues9 included an active control group of 358 high-risk women without BV and found that antibiotics did not improve perinatal outcomes in those patients.

As Flynn and colleagues point out, their result is disease-oriented evidence. Even those studies showing that antibiotic treatment reduces preterm deliveries do not address the ultimate patient-oriented outcome: the conditions of the neonate and the mother after delivery. Animal research has shown that using antibiotics to delay delivery in the presence of chorioamnionitis leads to fetal brain damage.11 Although women with BV do not have clinical chorioamnionitis, this data strikes a cautionary chord, suggesting that prolonging pregnancy in the setting of infection may not be the wisest course. Future studies must include data on the neonatal and postpartum sequelae of antibiotic treatment before we can be sure that we understand what the risks of treatment are and that they are outweighed by proven benefits.

Current guidelines

The American College of Obstetricians and Gynecologists suggests that screening for BV may be appropriate in women with a history of preterm delivery or who weigh less than 50 kg before pregnancy.12,13 Screening of other patients is not warranted on the basis of current evidence. BV can be treated after the first trimester with metronidazole 250 mg orally 3 times daily for 7 days or 500 mg orally twice daily for 7 days. Alternatives include metronidazole 2 g orally in a single dose or clindamycin 300 mg orally twice daily for 7 days. During the first trimester, symptomatic BV should be treated with clindamycin cream 2%, one applicatorful (5 g) intravaginally at bedtime for 7 days. Clindamycin can also be used orally during the first trimester, but the cream is preferred to minimize fetal exposure. However, vaginal therapy is not effective in preventing preterm delivery. There is no data regarding repeated screening or retreatment of persistent or recurrent BV.12-14

For now, physicians should consider prenatal screening and treatment for BV at the end of the second or the beginning of the third trimester in women with a history of preterm delivery (before 37 weeks’ gestation) or who weighed less than 50 kg before pregnancy. For all other patients, until larger, better-randomized studies of antibiotic treatment of BV during pregnancy become available, the answer to the question of screening remains “No.”

References

 

1. Gilbert D, Moellering R, Sande M. The Sanford guide to antimicrobial therapy. Vienna, Va: Antimicrobial Therapy, Inc; 1998.

2. Flynn CA, Helwig AL, Meurer LN. Bacterial vaginosis in pregnancy and the risk of prematurity: a meta-analysis. J Fam Pract 1999;48:885-892.

3. Hulley S, Grady D, Bush T, et al. Randomized trial of estrogen plus progestin for secondary prevention of coronary heart disease in postmenopausal women: Heart and Estrogen/progestin Replacement Study (HERS). JAMA 1998;280:605-13.

4. Duff P, Lee M, Hillier S, Herd L, Krohn M, Eschenbach D. Amoxicillin treatment of bacterial vaginosis during pregnancy. Obstet Gynecol 1991;77:431-5.

5. McGregor J, French J, Jones W, et al. Bacterial vaginosis is associated with prematurity and vaginal fluid mucinase and sialidase: results of a controlled trial of topical clindamycin cream. Am J Obstet Gynecol 1994;170:1048-60.

6. Joesof M, Hillier S, Wiknjosastro G, et al. Intravaginal clindamycin treatment for bacterial vaginosis: effects on preterm delivery and low birth weight. Am J Obstet Gynecol 1995;173:1527-31.

7. Gratacos E, Figueras F, Barranco M, et al. Spontaneous recovery of bacterial vaginosis during pregnancy is not associated with an improved perinatal outcome. Acta Obstet Gynecol Scand 1998;77:37-40.

8. Morales W, Schorr S, Albritton J. Effect of metronidazole in patients with preterm birth in preceding pregnancy and bacterial vaginosis: a placebo controlled double-blind study. Am J Obstet Gynecol 1994;171:345-9.

9. Hauth J, Goldenberg R, Andrews W, DuBard M, Copper R. Reduced incidence of preterm delivery with metronidazole and erythromycin in women with bacterial vaginosis. N Engl J Med 1995;333:1732-6.

10. McDonald H, O’Loughlin J, Vigneswaran R, et al. Impact of metronidazole therapy on preterm birth in women with bacterial vaginosis flora (Gardnerella vaginalis): a randomised, placebo controlled trial. Brit J Obstet Gynecol 1997;104:1391-7.

11. Brocklehurst P. Infection and preterm delivery. BMJ 1999;318:548-9.

12. Committee on Obstetric Practice Bacterial vaginosis screening for prevention of preterm delivery: ACOG committee opinion. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

13. Committee on Educational Bulletins Antimicrobial therapy for obstetric patients: ACOG educational bulletin. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

14. Centers for Disease Control and Prevention 1998 guidelines for treatment of sexually transmitted diseases. MMWR 1998;47:1-116.

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Bacterial vaginosis (BV) is a common condition in which the normal vaginal microflora are replaced by a polymicrobial overgrowth that includes Gardnerella vaginalis, Mycoplasma hominis, and anaerobes such as nonfragilis bacteroides, Mobiluncus, and peptococcus.1 It is now clear that bacterial vaginosis is associated with an increased risk of preterm delivery. The meta-analysis by Flynn and colleagues2 shows that the odds ratio of preterm delivery for patients with bacterial vaginosis during pregnancy is approximately 1.6. Although this is not an enormous increase in risk, it is both statistically and clinically significant. However, the association between BV and preterm delivery does not prove causation or that prenatal screening and treatment will improve perinatal outcomes.

Flynn and coworkers have carried out a detailed and thoughtful meta-analysis, but even a meta-analysis cannot overcome the inherent biases of the underlying case control and cohort studies which can not prove cause and effect. The Heart and Estrogen/Progestin Replacement Study3 demonstrated this phenomenon. That randomized placebo-controlled trial of postmenopausal hormone replacement therapy did not show the reduction in cardiac events that had been expected on the basis of previous observational case control and cohort data.

In the context of preterm delivery, BV is undoubtedly only a marker for something else—presumably subclinical infection of the upper genital tract—which then leads to preterm delivery. The combination of microbes that causes the upper tract infection is not known for certain. Studies in which the authors attempted to treat BV during pregnancy have shown no improvement in perinatal outcomes with oral amoxicillin4 or topical vaginal clindamycin,5,6 supporting the theory that anaerobic infection of the upper genital tract is the link between BV and preterm delivery. Spontaneous regression of BV during pregnancy assessed by vaginal gram stain also does not appear to improve perinatal outcomes, which again supports the idea that BV is not the direct cause of preterm delivery.

Three studies have shown that prenatal screening and treatment with oral metronidazole or with metronidazole and erythromycin seems to reduce the incidence of preterm delivery in patients with BV who also have other risk factors, such as a history of a previous preterm delivery or a low prepregnancy weight.8-10 However, 2 of these studies were weakened by methodologic problems8,10 or small sample numbers.10 These results need to be replicated in larger studies of high-risk women before they can be considered reliable. The case for screening and treating low-risk women is even less clear.

If BV is a marker for something else, would treating all high-risk women, even those without BV, also reduce the number of preterm deliveries? Hauth and colleagues9 included an active control group of 358 high-risk women without BV and found that antibiotics did not improve perinatal outcomes in those patients.

As Flynn and colleagues point out, their result is disease-oriented evidence. Even those studies showing that antibiotic treatment reduces preterm deliveries do not address the ultimate patient-oriented outcome: the conditions of the neonate and the mother after delivery. Animal research has shown that using antibiotics to delay delivery in the presence of chorioamnionitis leads to fetal brain damage.11 Although women with BV do not have clinical chorioamnionitis, this data strikes a cautionary chord, suggesting that prolonging pregnancy in the setting of infection may not be the wisest course. Future studies must include data on the neonatal and postpartum sequelae of antibiotic treatment before we can be sure that we understand what the risks of treatment are and that they are outweighed by proven benefits.

Current guidelines

The American College of Obstetricians and Gynecologists suggests that screening for BV may be appropriate in women with a history of preterm delivery or who weigh less than 50 kg before pregnancy.12,13 Screening of other patients is not warranted on the basis of current evidence. BV can be treated after the first trimester with metronidazole 250 mg orally 3 times daily for 7 days or 500 mg orally twice daily for 7 days. Alternatives include metronidazole 2 g orally in a single dose or clindamycin 300 mg orally twice daily for 7 days. During the first trimester, symptomatic BV should be treated with clindamycin cream 2%, one applicatorful (5 g) intravaginally at bedtime for 7 days. Clindamycin can also be used orally during the first trimester, but the cream is preferred to minimize fetal exposure. However, vaginal therapy is not effective in preventing preterm delivery. There is no data regarding repeated screening or retreatment of persistent or recurrent BV.12-14

For now, physicians should consider prenatal screening and treatment for BV at the end of the second or the beginning of the third trimester in women with a history of preterm delivery (before 37 weeks’ gestation) or who weighed less than 50 kg before pregnancy. For all other patients, until larger, better-randomized studies of antibiotic treatment of BV during pregnancy become available, the answer to the question of screening remains “No.”

Bacterial vaginosis (BV) is a common condition in which the normal vaginal microflora are replaced by a polymicrobial overgrowth that includes Gardnerella vaginalis, Mycoplasma hominis, and anaerobes such as nonfragilis bacteroides, Mobiluncus, and peptococcus.1 It is now clear that bacterial vaginosis is associated with an increased risk of preterm delivery. The meta-analysis by Flynn and colleagues2 shows that the odds ratio of preterm delivery for patients with bacterial vaginosis during pregnancy is approximately 1.6. Although this is not an enormous increase in risk, it is both statistically and clinically significant. However, the association between BV and preterm delivery does not prove causation or that prenatal screening and treatment will improve perinatal outcomes.

Flynn and coworkers have carried out a detailed and thoughtful meta-analysis, but even a meta-analysis cannot overcome the inherent biases of the underlying case control and cohort studies which can not prove cause and effect. The Heart and Estrogen/Progestin Replacement Study3 demonstrated this phenomenon. That randomized placebo-controlled trial of postmenopausal hormone replacement therapy did not show the reduction in cardiac events that had been expected on the basis of previous observational case control and cohort data.

In the context of preterm delivery, BV is undoubtedly only a marker for something else—presumably subclinical infection of the upper genital tract—which then leads to preterm delivery. The combination of microbes that causes the upper tract infection is not known for certain. Studies in which the authors attempted to treat BV during pregnancy have shown no improvement in perinatal outcomes with oral amoxicillin4 or topical vaginal clindamycin,5,6 supporting the theory that anaerobic infection of the upper genital tract is the link between BV and preterm delivery. Spontaneous regression of BV during pregnancy assessed by vaginal gram stain also does not appear to improve perinatal outcomes, which again supports the idea that BV is not the direct cause of preterm delivery.

Three studies have shown that prenatal screening and treatment with oral metronidazole or with metronidazole and erythromycin seems to reduce the incidence of preterm delivery in patients with BV who also have other risk factors, such as a history of a previous preterm delivery or a low prepregnancy weight.8-10 However, 2 of these studies were weakened by methodologic problems8,10 or small sample numbers.10 These results need to be replicated in larger studies of high-risk women before they can be considered reliable. The case for screening and treating low-risk women is even less clear.

If BV is a marker for something else, would treating all high-risk women, even those without BV, also reduce the number of preterm deliveries? Hauth and colleagues9 included an active control group of 358 high-risk women without BV and found that antibiotics did not improve perinatal outcomes in those patients.

As Flynn and colleagues point out, their result is disease-oriented evidence. Even those studies showing that antibiotic treatment reduces preterm deliveries do not address the ultimate patient-oriented outcome: the conditions of the neonate and the mother after delivery. Animal research has shown that using antibiotics to delay delivery in the presence of chorioamnionitis leads to fetal brain damage.11 Although women with BV do not have clinical chorioamnionitis, this data strikes a cautionary chord, suggesting that prolonging pregnancy in the setting of infection may not be the wisest course. Future studies must include data on the neonatal and postpartum sequelae of antibiotic treatment before we can be sure that we understand what the risks of treatment are and that they are outweighed by proven benefits.

Current guidelines

The American College of Obstetricians and Gynecologists suggests that screening for BV may be appropriate in women with a history of preterm delivery or who weigh less than 50 kg before pregnancy.12,13 Screening of other patients is not warranted on the basis of current evidence. BV can be treated after the first trimester with metronidazole 250 mg orally 3 times daily for 7 days or 500 mg orally twice daily for 7 days. Alternatives include metronidazole 2 g orally in a single dose or clindamycin 300 mg orally twice daily for 7 days. During the first trimester, symptomatic BV should be treated with clindamycin cream 2%, one applicatorful (5 g) intravaginally at bedtime for 7 days. Clindamycin can also be used orally during the first trimester, but the cream is preferred to minimize fetal exposure. However, vaginal therapy is not effective in preventing preterm delivery. There is no data regarding repeated screening or retreatment of persistent or recurrent BV.12-14

For now, physicians should consider prenatal screening and treatment for BV at the end of the second or the beginning of the third trimester in women with a history of preterm delivery (before 37 weeks’ gestation) or who weighed less than 50 kg before pregnancy. For all other patients, until larger, better-randomized studies of antibiotic treatment of BV during pregnancy become available, the answer to the question of screening remains “No.”

References

 

1. Gilbert D, Moellering R, Sande M. The Sanford guide to antimicrobial therapy. Vienna, Va: Antimicrobial Therapy, Inc; 1998.

2. Flynn CA, Helwig AL, Meurer LN. Bacterial vaginosis in pregnancy and the risk of prematurity: a meta-analysis. J Fam Pract 1999;48:885-892.

3. Hulley S, Grady D, Bush T, et al. Randomized trial of estrogen plus progestin for secondary prevention of coronary heart disease in postmenopausal women: Heart and Estrogen/progestin Replacement Study (HERS). JAMA 1998;280:605-13.

4. Duff P, Lee M, Hillier S, Herd L, Krohn M, Eschenbach D. Amoxicillin treatment of bacterial vaginosis during pregnancy. Obstet Gynecol 1991;77:431-5.

5. McGregor J, French J, Jones W, et al. Bacterial vaginosis is associated with prematurity and vaginal fluid mucinase and sialidase: results of a controlled trial of topical clindamycin cream. Am J Obstet Gynecol 1994;170:1048-60.

6. Joesof M, Hillier S, Wiknjosastro G, et al. Intravaginal clindamycin treatment for bacterial vaginosis: effects on preterm delivery and low birth weight. Am J Obstet Gynecol 1995;173:1527-31.

7. Gratacos E, Figueras F, Barranco M, et al. Spontaneous recovery of bacterial vaginosis during pregnancy is not associated with an improved perinatal outcome. Acta Obstet Gynecol Scand 1998;77:37-40.

8. Morales W, Schorr S, Albritton J. Effect of metronidazole in patients with preterm birth in preceding pregnancy and bacterial vaginosis: a placebo controlled double-blind study. Am J Obstet Gynecol 1994;171:345-9.

9. Hauth J, Goldenberg R, Andrews W, DuBard M, Copper R. Reduced incidence of preterm delivery with metronidazole and erythromycin in women with bacterial vaginosis. N Engl J Med 1995;333:1732-6.

10. McDonald H, O’Loughlin J, Vigneswaran R, et al. Impact of metronidazole therapy on preterm birth in women with bacterial vaginosis flora (Gardnerella vaginalis): a randomised, placebo controlled trial. Brit J Obstet Gynecol 1997;104:1391-7.

11. Brocklehurst P. Infection and preterm delivery. BMJ 1999;318:548-9.

12. Committee on Obstetric Practice Bacterial vaginosis screening for prevention of preterm delivery: ACOG committee opinion. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

13. Committee on Educational Bulletins Antimicrobial therapy for obstetric patients: ACOG educational bulletin. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

14. Centers for Disease Control and Prevention 1998 guidelines for treatment of sexually transmitted diseases. MMWR 1998;47:1-116.

References

 

1. Gilbert D, Moellering R, Sande M. The Sanford guide to antimicrobial therapy. Vienna, Va: Antimicrobial Therapy, Inc; 1998.

2. Flynn CA, Helwig AL, Meurer LN. Bacterial vaginosis in pregnancy and the risk of prematurity: a meta-analysis. J Fam Pract 1999;48:885-892.

3. Hulley S, Grady D, Bush T, et al. Randomized trial of estrogen plus progestin for secondary prevention of coronary heart disease in postmenopausal women: Heart and Estrogen/progestin Replacement Study (HERS). JAMA 1998;280:605-13.

4. Duff P, Lee M, Hillier S, Herd L, Krohn M, Eschenbach D. Amoxicillin treatment of bacterial vaginosis during pregnancy. Obstet Gynecol 1991;77:431-5.

5. McGregor J, French J, Jones W, et al. Bacterial vaginosis is associated with prematurity and vaginal fluid mucinase and sialidase: results of a controlled trial of topical clindamycin cream. Am J Obstet Gynecol 1994;170:1048-60.

6. Joesof M, Hillier S, Wiknjosastro G, et al. Intravaginal clindamycin treatment for bacterial vaginosis: effects on preterm delivery and low birth weight. Am J Obstet Gynecol 1995;173:1527-31.

7. Gratacos E, Figueras F, Barranco M, et al. Spontaneous recovery of bacterial vaginosis during pregnancy is not associated with an improved perinatal outcome. Acta Obstet Gynecol Scand 1998;77:37-40.

8. Morales W, Schorr S, Albritton J. Effect of metronidazole in patients with preterm birth in preceding pregnancy and bacterial vaginosis: a placebo controlled double-blind study. Am J Obstet Gynecol 1994;171:345-9.

9. Hauth J, Goldenberg R, Andrews W, DuBard M, Copper R. Reduced incidence of preterm delivery with metronidazole and erythromycin in women with bacterial vaginosis. N Engl J Med 1995;333:1732-6.

10. McDonald H, O’Loughlin J, Vigneswaran R, et al. Impact of metronidazole therapy on preterm birth in women with bacterial vaginosis flora (Gardnerella vaginalis): a randomised, placebo controlled trial. Brit J Obstet Gynecol 1997;104:1391-7.

11. Brocklehurst P. Infection and preterm delivery. BMJ 1999;318:548-9.

12. Committee on Obstetric Practice Bacterial vaginosis screening for prevention of preterm delivery: ACOG committee opinion. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

13. Committee on Educational Bulletins Antimicrobial therapy for obstetric patients: ACOG educational bulletin. Washington, DC: American College of Obstetricians and Gynecologists; 1998.

14. Centers for Disease Control and Prevention 1998 guidelines for treatment of sexually transmitted diseases. MMWR 1998;47:1-116.

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