Intrauterine fetal demise: Care in the aftermath, and beyond

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Intrauterine fetal demise: Care in the aftermath, and beyond

PRACTICE RECOMMENDATIONS

› Consider vaginal misoprostol for achieving delivery following intrauterine fetal demise (IUFD); it is as effective as other vaginal prostaglandin preparations and more effective than oral misoprostol. A
› Include in your postdelivery evaluation of IUFD autopsy, placental gross and histologic examination, fetal karyotype, and exam for fetomaternal hemorrhage. B
›Offer grieving parents early emotional support and counseling; research indicates it shortens the bereavement process.  A

Strength of recommendation (SOR)

A Good-quality patient-oriented evidence
B Inconsistent or limited-quality patient-oriented evidence
C Consensus, usual practice, opinion, disease-oriented evidence, case series

CASE › Louise T, age 26, is pregnant with her first child. She attends all prenatal care visits with her health care team and appears to be doing well. However, at Ms. T’s 28-week visit, her physician is unable to detect a fetal heartbeat, or any movement of the fetus. He orders an ultrasound, which confirms his suspicions. Ms. T opts for immediate induction of labor. In his postdelivery evaluation, Ms. T’s physician does not determine a definitive cause for the intrauterine fetal demise.

Intrauterine fetal demise (IUFD) is fetal death that occurs after 20 weeks gestation but before birth.1 If the gestational age is unknown at the time of death, a fetus that weighs ≥350 g is considered an IUFD. In 2005, IUFD occurred at a rate of 6.22 per 1000 pregnancies, which amounted to 25,894 deaths.1

Family physicians who provide obstetric care are likely to care for women who have experienced an IUFD. This article describes what that care should include.

Keep these risk factors in mind

IUFD has been attributed to an extensive range of risk factors and possible causes, including various maternal medical conditions, obstetric complications, and pathologic fetal or placental conditions (TABLE 1).2-8 The 2 most common risk factors—obesity (body mass index [BMI] >30) and smoking—are modifiable and increase the odds of IUFD approximately three-fold.2 Though less common, 2 other notable risk factors are lupus and chronic renal disease; their impact on IUFD risk varies depending on the severity of the disease.2 However, keep in mind that these factors may not be causal and that most pregnant women with these conditions will deliver healthy infants.

Induce labor, or wait?

A woman experiencing an IUFD is likely to seek care when she notices that the fetus isn’t moving or when she experiences contractions, loss of fluid, or vaginal bleeding. Alternatively, she could be asymptomatic, and it may be the physician who suspects IUFD when he/she is unable to hear fetal heart tones. The diagnosis is confirmed by the absence of fetal cardiac activity on ultrasound; physicians may wish to obtain a second ultrasound for confirmation of the diagnosis.

Up to 40% of unexplained cases of IUFD may actually be the result of an incomplete evaluation.Once IUFD is confirmed, most women choose to immediately undergo induction of labor. However, some elect to wait for spontaneous labor. Approximately 84% to 90% of women will go into spontaneous labor within 2 weeks of fetal death.9 Unless there is a compelling indication for immediate delivery (eg, coagulopathy, evidence of intrauterine infection, preeclampsia), expectant management may be permitted.

If a mother chooses expectant management, she should undergo periodic followup exams to assess for abdominal pain, fever, bleeding, bruising, labor, and emotional lability.10 Tell patients to seek immediate care if they develop a fever, abdominal pain, foul-smelling or purulent vaginal discharge, moderate bleeding, or bruising, or if they go into labor.

Vaginal prostaglandin effectively induces labor

Options for labor induction include oral or vaginal prostaglandins, continuous oxytocin infusion, or mechanical dilation (cervical placement of laminaria or a Foley bulb). Factors that affect which method to use include concomitant maternal illness, gestational age, Bishop score, or the presence of a uterine scar from a previous Cesarean section or other surgery. A Cochrane review found vaginal misoprostol was as effective as other vaginal prostaglandin preparations (E2 and F2-alpha) and more effective than oral misoprostol in achieving delivery for second- and third-trimester terminations and fetal deaths.11 Due to the risk of uterine rupture, most experts advise against use of misoprostol for a woman with a previously scarred uterus at >24 to 26 weeks gestation.10,12 In this circumstance, consider mechanical dilation followed by oxytocin infusion.

Beyond 28 weeks gestation, misoprostol can be used to induce labor by following the standard protocols utilized for term pregnancies (TABLE 2).10,12 Some patients may require additional doses of misoprostol to complete the third stage of labor. Pain can be managed via narcotic patient controlled analgesia, periodic use of intravenous narcotics, or continuous epidural.

 

 

A systematic approach to postdelivery evaluation

Although 25% to 60% of IUFDs are classified as “unexplained,” in up to 40% of cases the lack of explanation may be due to an incomplete evaluation.2-4 When performing an evaluation, it is important to be systematic and not confuse association with causality. Kortweg et al13 analyzed laboratory studies obtained in the evaluation of 1025 fetal deaths in the Netherlands from 2002 to 2008. The most useful tests were placental examination, fetal autopsy, and fetal karyotype, which aided in assigning the cause of death in 96%, 73%, and 29% of cases, respectively. Compared to fetal karyotyping from postpartum tissue sampling, samples obtained via amniocentesis or chorionic villus sampling before inducing labor are much more successful in identifying the cause of death (85% vs 28%).14

Testing for fetomaternal hemorrhage, which is the cause of IUFD about 12% of the time, needs to be performed when IUFD is diagnosed.13 Additional laboratory testing may be helpful depending on the mother’s history or symptoms at the time of IUFD. For example, a maternal history of drug use, thyroid disease, diabetes mellitus, hypertension, venous thromboembolism, or febrile illness should prompt further studies (TABLE 3).10,12-15

How to help grieving parents

Mothers may feel tremendous guilt upon suffering an IUFD. When addressing grief, mourning, and bereavement after an IUFD, the goal is to support the parents through the grieving process and properly identify when grief becomes pathologic. Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.16 In a prospective study, patient characteristics that affected the intensity of grief were advanced gestational age at loss, lack of children in the home, relatively older age, pre-loss neurotic personality, and pre-loss psychiatric symptoms.17

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated.

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated. Therefore, it is important for physicians to acknowledge that patients’ feelings of loss are legitimate. Additionally, reassure mothers that there was very likely nothing that she could have done to change the outcome, unless there is compelling evidence to the contrary (eg, drug abuse causing abruption and fetal demise). Avoid using phrases such as “you can always try again.”

In a study of 769 women who experienced an IUFD, many reported receiving “support” or “great support” from family members (91.7%), nurses (90%), and physicians (53.4%).18 Adequate health care support is associated with lower levels of depression and anxiety, but family support appears to be the most important.18 Women who are single, divorced, or widowed experience higher levels of depression after IUFD than those who are married or cohabitating.18

In a different study of support for women who experienced IUFD or death of their child shortly after birth, mothers did not blame doctors or feel that the doctors should make them feel better.19 However, they did want an explanation in simple language of what had gone wrong and for physicians to listen and accept their distress.19 This study also found that early support and counseling shortened the bereavement process.19 Half of women had symptoms of depression and anxiety 6 months after the death of their fetus or child and 20% had these symptoms at 14 months. Fathers, however, recovered more quickly—14% were symptomatic at 6 months.19

Managing a subsequent therapy

A retrospective cohort study found that for women who had experienced an IUFD, the odds ratio of having a recurrent IUFD was 1.94 (99% confidence interval, 1.29-2.92) compared to women who had a previous live birth.20 The risk of recurrent IUFD in a specific patient is related to the underlying pathophysiologic cause of the initial IUFD, and how that cause was addressed. For example, a patient who experienced an IUFD believed to be the result of uncontrolled diabetes can expect to have an improved outcome if her diabetes is brought under control before conceiving and she maintains control throughout the pregnancy. On the contrary, a patient who experienced an IUFD that was believed to be secondary to a nonmodifiable risk factor, such as lupus-induced chronic kidney disease, will continue to have a significant risk of recurrence of IUFD in the subsequent pregnancy.

Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.When managing a subsequent pregnancy of a woman who has experienced an IUFD, review all data from the prior pregnancy as well as the mother’s medical conditions. Order any studies in TABLE 3 that were not previously obtained and are clinically indicated. If applicable, encourage the woman to quite smoking and achieve a healthy BMI (<25).

 

 

In addition to routine obstetric care measures, these women should be offered antepartum fetal surveillance starting at 32 weeks gestation, or one to 2 weeks before the gestational age of the fetus at the time of the previous IUFD (whichever is earlier), as well as serial ultrasonography starting at 28 weeks to assess for fetal growth restriction.12,21 Most experts advise delivery at 39 weeks unless indicated earlier.12

Psychological risks. IUFD is associated with posttraumatic stress disorder (PTSD) and anxiety in a subsequent pregnancy.22,23 Approximately 21% of women in one There may be "false alarms" during the course of a woman's pregnancy if she's already experienced an IUFD.study met criteria for PTSD in the third trimester of the first subsequent pregnancy; this decreased to 4% at one year postpartum.22 Risk factors for PTSD and anxiety were conceiving within one year of IUFD and a perceived lack of support at time of loss.22,23 Additionally, women who said they had poor partner support at the time of IUFD were more likely to have more severe PTSD symptoms, such as recurring, involuntary distressing memories of the IUFD, 6 to 8 years later.24 Because women who become pregnant after having an IUFD are likely to be anxious, physicians should be aware that there may be “false alarms” during the course of these pregnancies.

CASE › Two years after experiencing an IUFD , Ms. T becomes pregnant. Her physician carefully reviews her medical records and begins fetal surveillance at 26 weeks gestation, including serial ultrasounds. Ms. T’s pregnancy and labor proceed without complications, and at 38 weeks, she delivers a healthy 6.3-lb. boy.

CORRESPONDENCE
Richard Temple, MD, Naval Hospital Camp Lejeune Family Medicine Residency, 100 Brewster Blvd., Camp Lejeune, NC 28547; richard.temple@med.navy.mil

ACKNOWLEDGMENT
The authors thank Anthony Viera, MD for his assistance in the preparation of this manuscript.

References

1. MacDorman MF, Kirmeyer S. Fetal and perinatal mortality, United States, 2005. Natl Vital Stat Rep. 2009;57:1-19.

2. Goldstein DP, Johnson JP, Reid DE. Management of intrauterine fetal death. Obstet Gynecol. 1963;21:523-529.

3. Fretts RC. Etiology and prevention of stillbirth. Am J Obstet Gynecol. 2005;193:1923-1935.

4. Huang DY, Usher RH, Kramer MS, et al. Determinants of unexplained antepartum fetal deaths. Obstet Gynecol. 2000;95:215-221.

5. Dudley DJ, Goldenberg R, Conway D, et al; Stillbirth Research Collaborative Network. A new system for determining the causes of stillbirth. Obstet Gynecol. 2010;116(2 pt 1):254-260.

6. Sims MA, Collins KA. Fetal death. A 10-year retrospective study. Am J Forensic Med Pathol. 2001;22:261-265.

7. Walsh CA, McMenamin MB, Foley ME, et al. Trends in intrapartum fetal death, 1979-2003. Am J Obstet Gynecol. 2008;198:47.e1-47.e7.

8. Smulian JC, Ananth CV, Vintzileos AM, et al. Fetal deaths in the United States. Influence of high-risk conditions and implications for management. Obstet Gynecol. 2002;100:1183-1189.

9. Silver RM. Fetal death. Obstet Gynecol. 2007;109:153-167.

10. Dodd JM, Crowther CA. Misoprostol for induction of labour to terminate pregnancy in the second or third trimester for women with a fetal anomaly or after intrauterine fetal death. Cochrane Database Syst Rev. 2010;(4):CD004901.

11. ACOG Practice Bulletin No. 102: management of stillbirth. Obstet Gynecol. 2009;113:748-761.

12. FrØen JF, Arnestad M, Frey K, et al. Risk factors for sudden intrauterine unexplained death: epidemiologic characteristics of singleton cases in Oslo, Norway, 1986-1995. Am J Obstet Gynecol. 2001;184:694-702.

13. Korteweg FJ, Erwich JJ, Timmer A, et al. Evaluation of 1025 fetal deaths: proposed diagnostic workup. Am J Obstet Gynecol. 2012;206:53.e1-53.e12.

14. Korteweg FJ, Bouman K, Erwich JJ, et al. Cytogenetic analysis after evaluation of 750 fetal deaths: proposal for diagnostic workup. Obstet Gynecol. 2008;111:865-874.

15. Silver RM, Varner MW, Reddy U, et al. Work-up of stillbirth: a review of the literature. Am J Obstet Gynecol. 2007;196:433-444.

16. Badenhorst W, Hughes P. Psychological aspects of perinatal loss. Best Pract Res Clin Obstet Gynaecol. 2007;21:249-259.

17. Janssen HJ, Cuisinier MC, de Graauw KP, et al. A prospective study of risk factors predicting grief intensity following pregnancy loss. Arch Gen Psychiatry. 1997;54:56-61.

18. Cacciatore J, Schnebly S, Froen JF. The effects of social support on maternal anxiety and depression after stillbirth. Health Soc Care Community. 2009;17:167-176.

19. Forrest GC, Standish E, Baum JD. Support after perinatal death: a study of support and counselling after perinatal bereavement. Br Med J (Clin Res Ed). 1982;285:1475-1479.

20. Bhattacharya S, Prescott GJ, Black M, et al. Recurrence risk of stillbirth in a second pregnancy. BJOG. 2010;117:1243-1247.

21. Reddy UM. Management of pregnancy after stillbirth. Clin Obstet Gynecol. 2010;53:700-709.

22. Turton P, Hughes P, Evans CD, et al. Incidence, correlates and predictors of post-traumatic stress disorder in the pregnancy after stillbirth. Br J Psychiatry. 2001;178:556-560.

23. Hughes PM, Turton P, Evans CD. Stillbirth as risk factor for depression and anxiety in the subsequent pregnancy: cohort study. BMJ. 1999;318:1721-1724.

24. Turton P, Evans C, Hughes P. Long-term psychosocial sequelae of stillbirth: phase II of a nested case-control cohort study. Arch Womens Ment Health. 2009;12:35-41.

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Richard Temple, MD
Stephanie Smith, MD

Naval Hospital Camp Lejune Family Medicine Residency, Camp Lejeune, NC
richard.temple@med.navy.mil

The authors reported no potential conflict of interest relevant to this article.

The views expressed in this article are those of the authors and do not necessarily reflect the official policy or position of the Department of the Navy, Department of Defense, or the US Government.

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Richard Temple; MD; Stephanie Smith; MD; IUFD; intrauterine fetal demise; pregnancy; labor; misoprostol; post delivery; grief; testing
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Richard Temple, MD
Stephanie Smith, MD

Naval Hospital Camp Lejune Family Medicine Residency, Camp Lejeune, NC
richard.temple@med.navy.mil

The authors reported no potential conflict of interest relevant to this article.

The views expressed in this article are those of the authors and do not necessarily reflect the official policy or position of the Department of the Navy, Department of Defense, or the US Government.

Author and Disclosure Information

Richard Temple, MD
Stephanie Smith, MD

Naval Hospital Camp Lejune Family Medicine Residency, Camp Lejeune, NC
richard.temple@med.navy.mil

The authors reported no potential conflict of interest relevant to this article.

The views expressed in this article are those of the authors and do not necessarily reflect the official policy or position of the Department of the Navy, Department of Defense, or the US Government.

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PRACTICE RECOMMENDATIONS

› Consider vaginal misoprostol for achieving delivery following intrauterine fetal demise (IUFD); it is as effective as other vaginal prostaglandin preparations and more effective than oral misoprostol. A
› Include in your postdelivery evaluation of IUFD autopsy, placental gross and histologic examination, fetal karyotype, and exam for fetomaternal hemorrhage. B
›Offer grieving parents early emotional support and counseling; research indicates it shortens the bereavement process.  A

Strength of recommendation (SOR)

A Good-quality patient-oriented evidence
B Inconsistent or limited-quality patient-oriented evidence
C Consensus, usual practice, opinion, disease-oriented evidence, case series

CASE › Louise T, age 26, is pregnant with her first child. She attends all prenatal care visits with her health care team and appears to be doing well. However, at Ms. T’s 28-week visit, her physician is unable to detect a fetal heartbeat, or any movement of the fetus. He orders an ultrasound, which confirms his suspicions. Ms. T opts for immediate induction of labor. In his postdelivery evaluation, Ms. T’s physician does not determine a definitive cause for the intrauterine fetal demise.

Intrauterine fetal demise (IUFD) is fetal death that occurs after 20 weeks gestation but before birth.1 If the gestational age is unknown at the time of death, a fetus that weighs ≥350 g is considered an IUFD. In 2005, IUFD occurred at a rate of 6.22 per 1000 pregnancies, which amounted to 25,894 deaths.1

Family physicians who provide obstetric care are likely to care for women who have experienced an IUFD. This article describes what that care should include.

Keep these risk factors in mind

IUFD has been attributed to an extensive range of risk factors and possible causes, including various maternal medical conditions, obstetric complications, and pathologic fetal or placental conditions (TABLE 1).2-8 The 2 most common risk factors—obesity (body mass index [BMI] >30) and smoking—are modifiable and increase the odds of IUFD approximately three-fold.2 Though less common, 2 other notable risk factors are lupus and chronic renal disease; their impact on IUFD risk varies depending on the severity of the disease.2 However, keep in mind that these factors may not be causal and that most pregnant women with these conditions will deliver healthy infants.

Induce labor, or wait?

A woman experiencing an IUFD is likely to seek care when she notices that the fetus isn’t moving or when she experiences contractions, loss of fluid, or vaginal bleeding. Alternatively, she could be asymptomatic, and it may be the physician who suspects IUFD when he/she is unable to hear fetal heart tones. The diagnosis is confirmed by the absence of fetal cardiac activity on ultrasound; physicians may wish to obtain a second ultrasound for confirmation of the diagnosis.

Up to 40% of unexplained cases of IUFD may actually be the result of an incomplete evaluation.Once IUFD is confirmed, most women choose to immediately undergo induction of labor. However, some elect to wait for spontaneous labor. Approximately 84% to 90% of women will go into spontaneous labor within 2 weeks of fetal death.9 Unless there is a compelling indication for immediate delivery (eg, coagulopathy, evidence of intrauterine infection, preeclampsia), expectant management may be permitted.

If a mother chooses expectant management, she should undergo periodic followup exams to assess for abdominal pain, fever, bleeding, bruising, labor, and emotional lability.10 Tell patients to seek immediate care if they develop a fever, abdominal pain, foul-smelling or purulent vaginal discharge, moderate bleeding, or bruising, or if they go into labor.

Vaginal prostaglandin effectively induces labor

Options for labor induction include oral or vaginal prostaglandins, continuous oxytocin infusion, or mechanical dilation (cervical placement of laminaria or a Foley bulb). Factors that affect which method to use include concomitant maternal illness, gestational age, Bishop score, or the presence of a uterine scar from a previous Cesarean section or other surgery. A Cochrane review found vaginal misoprostol was as effective as other vaginal prostaglandin preparations (E2 and F2-alpha) and more effective than oral misoprostol in achieving delivery for second- and third-trimester terminations and fetal deaths.11 Due to the risk of uterine rupture, most experts advise against use of misoprostol for a woman with a previously scarred uterus at >24 to 26 weeks gestation.10,12 In this circumstance, consider mechanical dilation followed by oxytocin infusion.

Beyond 28 weeks gestation, misoprostol can be used to induce labor by following the standard protocols utilized for term pregnancies (TABLE 2).10,12 Some patients may require additional doses of misoprostol to complete the third stage of labor. Pain can be managed via narcotic patient controlled analgesia, periodic use of intravenous narcotics, or continuous epidural.

 

 

A systematic approach to postdelivery evaluation

Although 25% to 60% of IUFDs are classified as “unexplained,” in up to 40% of cases the lack of explanation may be due to an incomplete evaluation.2-4 When performing an evaluation, it is important to be systematic and not confuse association with causality. Kortweg et al13 analyzed laboratory studies obtained in the evaluation of 1025 fetal deaths in the Netherlands from 2002 to 2008. The most useful tests were placental examination, fetal autopsy, and fetal karyotype, which aided in assigning the cause of death in 96%, 73%, and 29% of cases, respectively. Compared to fetal karyotyping from postpartum tissue sampling, samples obtained via amniocentesis or chorionic villus sampling before inducing labor are much more successful in identifying the cause of death (85% vs 28%).14

Testing for fetomaternal hemorrhage, which is the cause of IUFD about 12% of the time, needs to be performed when IUFD is diagnosed.13 Additional laboratory testing may be helpful depending on the mother’s history or symptoms at the time of IUFD. For example, a maternal history of drug use, thyroid disease, diabetes mellitus, hypertension, venous thromboembolism, or febrile illness should prompt further studies (TABLE 3).10,12-15

How to help grieving parents

Mothers may feel tremendous guilt upon suffering an IUFD. When addressing grief, mourning, and bereavement after an IUFD, the goal is to support the parents through the grieving process and properly identify when grief becomes pathologic. Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.16 In a prospective study, patient characteristics that affected the intensity of grief were advanced gestational age at loss, lack of children in the home, relatively older age, pre-loss neurotic personality, and pre-loss psychiatric symptoms.17

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated.

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated. Therefore, it is important for physicians to acknowledge that patients’ feelings of loss are legitimate. Additionally, reassure mothers that there was very likely nothing that she could have done to change the outcome, unless there is compelling evidence to the contrary (eg, drug abuse causing abruption and fetal demise). Avoid using phrases such as “you can always try again.”

In a study of 769 women who experienced an IUFD, many reported receiving “support” or “great support” from family members (91.7%), nurses (90%), and physicians (53.4%).18 Adequate health care support is associated with lower levels of depression and anxiety, but family support appears to be the most important.18 Women who are single, divorced, or widowed experience higher levels of depression after IUFD than those who are married or cohabitating.18

In a different study of support for women who experienced IUFD or death of their child shortly after birth, mothers did not blame doctors or feel that the doctors should make them feel better.19 However, they did want an explanation in simple language of what had gone wrong and for physicians to listen and accept their distress.19 This study also found that early support and counseling shortened the bereavement process.19 Half of women had symptoms of depression and anxiety 6 months after the death of their fetus or child and 20% had these symptoms at 14 months. Fathers, however, recovered more quickly—14% were symptomatic at 6 months.19

Managing a subsequent therapy

A retrospective cohort study found that for women who had experienced an IUFD, the odds ratio of having a recurrent IUFD was 1.94 (99% confidence interval, 1.29-2.92) compared to women who had a previous live birth.20 The risk of recurrent IUFD in a specific patient is related to the underlying pathophysiologic cause of the initial IUFD, and how that cause was addressed. For example, a patient who experienced an IUFD believed to be the result of uncontrolled diabetes can expect to have an improved outcome if her diabetes is brought under control before conceiving and she maintains control throughout the pregnancy. On the contrary, a patient who experienced an IUFD that was believed to be secondary to a nonmodifiable risk factor, such as lupus-induced chronic kidney disease, will continue to have a significant risk of recurrence of IUFD in the subsequent pregnancy.

Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.When managing a subsequent pregnancy of a woman who has experienced an IUFD, review all data from the prior pregnancy as well as the mother’s medical conditions. Order any studies in TABLE 3 that were not previously obtained and are clinically indicated. If applicable, encourage the woman to quite smoking and achieve a healthy BMI (<25).

 

 

In addition to routine obstetric care measures, these women should be offered antepartum fetal surveillance starting at 32 weeks gestation, or one to 2 weeks before the gestational age of the fetus at the time of the previous IUFD (whichever is earlier), as well as serial ultrasonography starting at 28 weeks to assess for fetal growth restriction.12,21 Most experts advise delivery at 39 weeks unless indicated earlier.12

Psychological risks. IUFD is associated with posttraumatic stress disorder (PTSD) and anxiety in a subsequent pregnancy.22,23 Approximately 21% of women in one There may be "false alarms" during the course of a woman's pregnancy if she's already experienced an IUFD.study met criteria for PTSD in the third trimester of the first subsequent pregnancy; this decreased to 4% at one year postpartum.22 Risk factors for PTSD and anxiety were conceiving within one year of IUFD and a perceived lack of support at time of loss.22,23 Additionally, women who said they had poor partner support at the time of IUFD were more likely to have more severe PTSD symptoms, such as recurring, involuntary distressing memories of the IUFD, 6 to 8 years later.24 Because women who become pregnant after having an IUFD are likely to be anxious, physicians should be aware that there may be “false alarms” during the course of these pregnancies.

CASE › Two years after experiencing an IUFD , Ms. T becomes pregnant. Her physician carefully reviews her medical records and begins fetal surveillance at 26 weeks gestation, including serial ultrasounds. Ms. T’s pregnancy and labor proceed without complications, and at 38 weeks, she delivers a healthy 6.3-lb. boy.

CORRESPONDENCE
Richard Temple, MD, Naval Hospital Camp Lejeune Family Medicine Residency, 100 Brewster Blvd., Camp Lejeune, NC 28547; richard.temple@med.navy.mil

ACKNOWLEDGMENT
The authors thank Anthony Viera, MD for his assistance in the preparation of this manuscript.

PRACTICE RECOMMENDATIONS

› Consider vaginal misoprostol for achieving delivery following intrauterine fetal demise (IUFD); it is as effective as other vaginal prostaglandin preparations and more effective than oral misoprostol. A
› Include in your postdelivery evaluation of IUFD autopsy, placental gross and histologic examination, fetal karyotype, and exam for fetomaternal hemorrhage. B
›Offer grieving parents early emotional support and counseling; research indicates it shortens the bereavement process.  A

Strength of recommendation (SOR)

A Good-quality patient-oriented evidence
B Inconsistent or limited-quality patient-oriented evidence
C Consensus, usual practice, opinion, disease-oriented evidence, case series

CASE › Louise T, age 26, is pregnant with her first child. She attends all prenatal care visits with her health care team and appears to be doing well. However, at Ms. T’s 28-week visit, her physician is unable to detect a fetal heartbeat, or any movement of the fetus. He orders an ultrasound, which confirms his suspicions. Ms. T opts for immediate induction of labor. In his postdelivery evaluation, Ms. T’s physician does not determine a definitive cause for the intrauterine fetal demise.

Intrauterine fetal demise (IUFD) is fetal death that occurs after 20 weeks gestation but before birth.1 If the gestational age is unknown at the time of death, a fetus that weighs ≥350 g is considered an IUFD. In 2005, IUFD occurred at a rate of 6.22 per 1000 pregnancies, which amounted to 25,894 deaths.1

Family physicians who provide obstetric care are likely to care for women who have experienced an IUFD. This article describes what that care should include.

Keep these risk factors in mind

IUFD has been attributed to an extensive range of risk factors and possible causes, including various maternal medical conditions, obstetric complications, and pathologic fetal or placental conditions (TABLE 1).2-8 The 2 most common risk factors—obesity (body mass index [BMI] >30) and smoking—are modifiable and increase the odds of IUFD approximately three-fold.2 Though less common, 2 other notable risk factors are lupus and chronic renal disease; their impact on IUFD risk varies depending on the severity of the disease.2 However, keep in mind that these factors may not be causal and that most pregnant women with these conditions will deliver healthy infants.

Induce labor, or wait?

A woman experiencing an IUFD is likely to seek care when she notices that the fetus isn’t moving or when she experiences contractions, loss of fluid, or vaginal bleeding. Alternatively, she could be asymptomatic, and it may be the physician who suspects IUFD when he/she is unable to hear fetal heart tones. The diagnosis is confirmed by the absence of fetal cardiac activity on ultrasound; physicians may wish to obtain a second ultrasound for confirmation of the diagnosis.

Up to 40% of unexplained cases of IUFD may actually be the result of an incomplete evaluation.Once IUFD is confirmed, most women choose to immediately undergo induction of labor. However, some elect to wait for spontaneous labor. Approximately 84% to 90% of women will go into spontaneous labor within 2 weeks of fetal death.9 Unless there is a compelling indication for immediate delivery (eg, coagulopathy, evidence of intrauterine infection, preeclampsia), expectant management may be permitted.

If a mother chooses expectant management, she should undergo periodic followup exams to assess for abdominal pain, fever, bleeding, bruising, labor, and emotional lability.10 Tell patients to seek immediate care if they develop a fever, abdominal pain, foul-smelling or purulent vaginal discharge, moderate bleeding, or bruising, or if they go into labor.

Vaginal prostaglandin effectively induces labor

Options for labor induction include oral or vaginal prostaglandins, continuous oxytocin infusion, or mechanical dilation (cervical placement of laminaria or a Foley bulb). Factors that affect which method to use include concomitant maternal illness, gestational age, Bishop score, or the presence of a uterine scar from a previous Cesarean section or other surgery. A Cochrane review found vaginal misoprostol was as effective as other vaginal prostaglandin preparations (E2 and F2-alpha) and more effective than oral misoprostol in achieving delivery for second- and third-trimester terminations and fetal deaths.11 Due to the risk of uterine rupture, most experts advise against use of misoprostol for a woman with a previously scarred uterus at >24 to 26 weeks gestation.10,12 In this circumstance, consider mechanical dilation followed by oxytocin infusion.

Beyond 28 weeks gestation, misoprostol can be used to induce labor by following the standard protocols utilized for term pregnancies (TABLE 2).10,12 Some patients may require additional doses of misoprostol to complete the third stage of labor. Pain can be managed via narcotic patient controlled analgesia, periodic use of intravenous narcotics, or continuous epidural.

 

 

A systematic approach to postdelivery evaluation

Although 25% to 60% of IUFDs are classified as “unexplained,” in up to 40% of cases the lack of explanation may be due to an incomplete evaluation.2-4 When performing an evaluation, it is important to be systematic and not confuse association with causality. Kortweg et al13 analyzed laboratory studies obtained in the evaluation of 1025 fetal deaths in the Netherlands from 2002 to 2008. The most useful tests were placental examination, fetal autopsy, and fetal karyotype, which aided in assigning the cause of death in 96%, 73%, and 29% of cases, respectively. Compared to fetal karyotyping from postpartum tissue sampling, samples obtained via amniocentesis or chorionic villus sampling before inducing labor are much more successful in identifying the cause of death (85% vs 28%).14

Testing for fetomaternal hemorrhage, which is the cause of IUFD about 12% of the time, needs to be performed when IUFD is diagnosed.13 Additional laboratory testing may be helpful depending on the mother’s history or symptoms at the time of IUFD. For example, a maternal history of drug use, thyroid disease, diabetes mellitus, hypertension, venous thromboembolism, or febrile illness should prompt further studies (TABLE 3).10,12-15

How to help grieving parents

Mothers may feel tremendous guilt upon suffering an IUFD. When addressing grief, mourning, and bereavement after an IUFD, the goal is to support the parents through the grieving process and properly identify when grief becomes pathologic. Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.16 In a prospective study, patient characteristics that affected the intensity of grief were advanced gestational age at loss, lack of children in the home, relatively older age, pre-loss neurotic personality, and pre-loss psychiatric symptoms.17

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated.

Unlike the grief experienced by parents who lose an infant or child, the grief experienced by parents who experience an IUFD may not be socially validated. Therefore, it is important for physicians to acknowledge that patients’ feelings of loss are legitimate. Additionally, reassure mothers that there was very likely nothing that she could have done to change the outcome, unless there is compelling evidence to the contrary (eg, drug abuse causing abruption and fetal demise). Avoid using phrases such as “you can always try again.”

In a study of 769 women who experienced an IUFD, many reported receiving “support” or “great support” from family members (91.7%), nurses (90%), and physicians (53.4%).18 Adequate health care support is associated with lower levels of depression and anxiety, but family support appears to be the most important.18 Women who are single, divorced, or widowed experience higher levels of depression after IUFD than those who are married or cohabitating.18

In a different study of support for women who experienced IUFD or death of their child shortly after birth, mothers did not blame doctors or feel that the doctors should make them feel better.19 However, they did want an explanation in simple language of what had gone wrong and for physicians to listen and accept their distress.19 This study also found that early support and counseling shortened the bereavement process.19 Half of women had symptoms of depression and anxiety 6 months after the death of their fetus or child and 20% had these symptoms at 14 months. Fathers, however, recovered more quickly—14% were symptomatic at 6 months.19

Managing a subsequent therapy

A retrospective cohort study found that for women who had experienced an IUFD, the odds ratio of having a recurrent IUFD was 1.94 (99% confidence interval, 1.29-2.92) compared to women who had a previous live birth.20 The risk of recurrent IUFD in a specific patient is related to the underlying pathophysiologic cause of the initial IUFD, and how that cause was addressed. For example, a patient who experienced an IUFD believed to be the result of uncontrolled diabetes can expect to have an improved outcome if her diabetes is brought under control before conceiving and she maintains control throughout the pregnancy. On the contrary, a patient who experienced an IUFD that was believed to be secondary to a nonmodifiable risk factor, such as lupus-induced chronic kidney disease, will continue to have a significant risk of recurrence of IUFD in the subsequent pregnancy.

Grief is pathologic when there is a prolonged response—usually longer than 6 months—and when it interferes with daily activities.When managing a subsequent pregnancy of a woman who has experienced an IUFD, review all data from the prior pregnancy as well as the mother’s medical conditions. Order any studies in TABLE 3 that were not previously obtained and are clinically indicated. If applicable, encourage the woman to quite smoking and achieve a healthy BMI (<25).

 

 

In addition to routine obstetric care measures, these women should be offered antepartum fetal surveillance starting at 32 weeks gestation, or one to 2 weeks before the gestational age of the fetus at the time of the previous IUFD (whichever is earlier), as well as serial ultrasonography starting at 28 weeks to assess for fetal growth restriction.12,21 Most experts advise delivery at 39 weeks unless indicated earlier.12

Psychological risks. IUFD is associated with posttraumatic stress disorder (PTSD) and anxiety in a subsequent pregnancy.22,23 Approximately 21% of women in one There may be "false alarms" during the course of a woman's pregnancy if she's already experienced an IUFD.study met criteria for PTSD in the third trimester of the first subsequent pregnancy; this decreased to 4% at one year postpartum.22 Risk factors for PTSD and anxiety were conceiving within one year of IUFD and a perceived lack of support at time of loss.22,23 Additionally, women who said they had poor partner support at the time of IUFD were more likely to have more severe PTSD symptoms, such as recurring, involuntary distressing memories of the IUFD, 6 to 8 years later.24 Because women who become pregnant after having an IUFD are likely to be anxious, physicians should be aware that there may be “false alarms” during the course of these pregnancies.

CASE › Two years after experiencing an IUFD , Ms. T becomes pregnant. Her physician carefully reviews her medical records and begins fetal surveillance at 26 weeks gestation, including serial ultrasounds. Ms. T’s pregnancy and labor proceed without complications, and at 38 weeks, she delivers a healthy 6.3-lb. boy.

CORRESPONDENCE
Richard Temple, MD, Naval Hospital Camp Lejeune Family Medicine Residency, 100 Brewster Blvd., Camp Lejeune, NC 28547; richard.temple@med.navy.mil

ACKNOWLEDGMENT
The authors thank Anthony Viera, MD for his assistance in the preparation of this manuscript.

References

1. MacDorman MF, Kirmeyer S. Fetal and perinatal mortality, United States, 2005. Natl Vital Stat Rep. 2009;57:1-19.

2. Goldstein DP, Johnson JP, Reid DE. Management of intrauterine fetal death. Obstet Gynecol. 1963;21:523-529.

3. Fretts RC. Etiology and prevention of stillbirth. Am J Obstet Gynecol. 2005;193:1923-1935.

4. Huang DY, Usher RH, Kramer MS, et al. Determinants of unexplained antepartum fetal deaths. Obstet Gynecol. 2000;95:215-221.

5. Dudley DJ, Goldenberg R, Conway D, et al; Stillbirth Research Collaborative Network. A new system for determining the causes of stillbirth. Obstet Gynecol. 2010;116(2 pt 1):254-260.

6. Sims MA, Collins KA. Fetal death. A 10-year retrospective study. Am J Forensic Med Pathol. 2001;22:261-265.

7. Walsh CA, McMenamin MB, Foley ME, et al. Trends in intrapartum fetal death, 1979-2003. Am J Obstet Gynecol. 2008;198:47.e1-47.e7.

8. Smulian JC, Ananth CV, Vintzileos AM, et al. Fetal deaths in the United States. Influence of high-risk conditions and implications for management. Obstet Gynecol. 2002;100:1183-1189.

9. Silver RM. Fetal death. Obstet Gynecol. 2007;109:153-167.

10. Dodd JM, Crowther CA. Misoprostol for induction of labour to terminate pregnancy in the second or third trimester for women with a fetal anomaly or after intrauterine fetal death. Cochrane Database Syst Rev. 2010;(4):CD004901.

11. ACOG Practice Bulletin No. 102: management of stillbirth. Obstet Gynecol. 2009;113:748-761.

12. FrØen JF, Arnestad M, Frey K, et al. Risk factors for sudden intrauterine unexplained death: epidemiologic characteristics of singleton cases in Oslo, Norway, 1986-1995. Am J Obstet Gynecol. 2001;184:694-702.

13. Korteweg FJ, Erwich JJ, Timmer A, et al. Evaluation of 1025 fetal deaths: proposed diagnostic workup. Am J Obstet Gynecol. 2012;206:53.e1-53.e12.

14. Korteweg FJ, Bouman K, Erwich JJ, et al. Cytogenetic analysis after evaluation of 750 fetal deaths: proposal for diagnostic workup. Obstet Gynecol. 2008;111:865-874.

15. Silver RM, Varner MW, Reddy U, et al. Work-up of stillbirth: a review of the literature. Am J Obstet Gynecol. 2007;196:433-444.

16. Badenhorst W, Hughes P. Psychological aspects of perinatal loss. Best Pract Res Clin Obstet Gynaecol. 2007;21:249-259.

17. Janssen HJ, Cuisinier MC, de Graauw KP, et al. A prospective study of risk factors predicting grief intensity following pregnancy loss. Arch Gen Psychiatry. 1997;54:56-61.

18. Cacciatore J, Schnebly S, Froen JF. The effects of social support on maternal anxiety and depression after stillbirth. Health Soc Care Community. 2009;17:167-176.

19. Forrest GC, Standish E, Baum JD. Support after perinatal death: a study of support and counselling after perinatal bereavement. Br Med J (Clin Res Ed). 1982;285:1475-1479.

20. Bhattacharya S, Prescott GJ, Black M, et al. Recurrence risk of stillbirth in a second pregnancy. BJOG. 2010;117:1243-1247.

21. Reddy UM. Management of pregnancy after stillbirth. Clin Obstet Gynecol. 2010;53:700-709.

22. Turton P, Hughes P, Evans CD, et al. Incidence, correlates and predictors of post-traumatic stress disorder in the pregnancy after stillbirth. Br J Psychiatry. 2001;178:556-560.

23. Hughes PM, Turton P, Evans CD. Stillbirth as risk factor for depression and anxiety in the subsequent pregnancy: cohort study. BMJ. 1999;318:1721-1724.

24. Turton P, Evans C, Hughes P. Long-term psychosocial sequelae of stillbirth: phase II of a nested case-control cohort study. Arch Womens Ment Health. 2009;12:35-41.

References

1. MacDorman MF, Kirmeyer S. Fetal and perinatal mortality, United States, 2005. Natl Vital Stat Rep. 2009;57:1-19.

2. Goldstein DP, Johnson JP, Reid DE. Management of intrauterine fetal death. Obstet Gynecol. 1963;21:523-529.

3. Fretts RC. Etiology and prevention of stillbirth. Am J Obstet Gynecol. 2005;193:1923-1935.

4. Huang DY, Usher RH, Kramer MS, et al. Determinants of unexplained antepartum fetal deaths. Obstet Gynecol. 2000;95:215-221.

5. Dudley DJ, Goldenberg R, Conway D, et al; Stillbirth Research Collaborative Network. A new system for determining the causes of stillbirth. Obstet Gynecol. 2010;116(2 pt 1):254-260.

6. Sims MA, Collins KA. Fetal death. A 10-year retrospective study. Am J Forensic Med Pathol. 2001;22:261-265.

7. Walsh CA, McMenamin MB, Foley ME, et al. Trends in intrapartum fetal death, 1979-2003. Am J Obstet Gynecol. 2008;198:47.e1-47.e7.

8. Smulian JC, Ananth CV, Vintzileos AM, et al. Fetal deaths in the United States. Influence of high-risk conditions and implications for management. Obstet Gynecol. 2002;100:1183-1189.

9. Silver RM. Fetal death. Obstet Gynecol. 2007;109:153-167.

10. Dodd JM, Crowther CA. Misoprostol for induction of labour to terminate pregnancy in the second or third trimester for women with a fetal anomaly or after intrauterine fetal death. Cochrane Database Syst Rev. 2010;(4):CD004901.

11. ACOG Practice Bulletin No. 102: management of stillbirth. Obstet Gynecol. 2009;113:748-761.

12. FrØen JF, Arnestad M, Frey K, et al. Risk factors for sudden intrauterine unexplained death: epidemiologic characteristics of singleton cases in Oslo, Norway, 1986-1995. Am J Obstet Gynecol. 2001;184:694-702.

13. Korteweg FJ, Erwich JJ, Timmer A, et al. Evaluation of 1025 fetal deaths: proposed diagnostic workup. Am J Obstet Gynecol. 2012;206:53.e1-53.e12.

14. Korteweg FJ, Bouman K, Erwich JJ, et al. Cytogenetic analysis after evaluation of 750 fetal deaths: proposal for diagnostic workup. Obstet Gynecol. 2008;111:865-874.

15. Silver RM, Varner MW, Reddy U, et al. Work-up of stillbirth: a review of the literature. Am J Obstet Gynecol. 2007;196:433-444.

16. Badenhorst W, Hughes P. Psychological aspects of perinatal loss. Best Pract Res Clin Obstet Gynaecol. 2007;21:249-259.

17. Janssen HJ, Cuisinier MC, de Graauw KP, et al. A prospective study of risk factors predicting grief intensity following pregnancy loss. Arch Gen Psychiatry. 1997;54:56-61.

18. Cacciatore J, Schnebly S, Froen JF. The effects of social support on maternal anxiety and depression after stillbirth. Health Soc Care Community. 2009;17:167-176.

19. Forrest GC, Standish E, Baum JD. Support after perinatal death: a study of support and counselling after perinatal bereavement. Br Med J (Clin Res Ed). 1982;285:1475-1479.

20. Bhattacharya S, Prescott GJ, Black M, et al. Recurrence risk of stillbirth in a second pregnancy. BJOG. 2010;117:1243-1247.

21. Reddy UM. Management of pregnancy after stillbirth. Clin Obstet Gynecol. 2010;53:700-709.

22. Turton P, Hughes P, Evans CD, et al. Incidence, correlates and predictors of post-traumatic stress disorder in the pregnancy after stillbirth. Br J Psychiatry. 2001;178:556-560.

23. Hughes PM, Turton P, Evans CD. Stillbirth as risk factor for depression and anxiety in the subsequent pregnancy: cohort study. BMJ. 1999;318:1721-1724.

24. Turton P, Evans C, Hughes P. Long-term psychosocial sequelae of stillbirth: phase II of a nested case-control cohort study. Arch Womens Ment Health. 2009;12:35-41.

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The Journal of Family Practice - 63(6)
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The Journal of Family Practice - 63(6)
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Intrauterine fetal demise: Care in the aftermath, and beyond
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Intrauterine fetal demise: Care in the aftermath, and beyond
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Richard Temple; MD; Stephanie Smith; MD; IUFD; intrauterine fetal demise; pregnancy; labor; misoprostol; post delivery; grief; testing
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Richard Temple; MD; Stephanie Smith; MD; IUFD; intrauterine fetal demise; pregnancy; labor; misoprostol; post delivery; grief; testing
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