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A female liver transplant recipient asks: Can I become pregnant?
Author(s)
Lydia Chelala, MD
Ghassan Ilaiwy, MD
Ibrahim A. Hanouneh, MD

Yes, pregnancy is possible, but not immediately after transplant, and it involves risks. Appropriate management and multidisciplinary care are necessary to optimize the outcomes.

HOW LONG SHOULD PREGNANCY BE POSTPONED?

Hypogonadism and amenorrhea are common and multifactorial in women with end-stage liver disease. Hypogonadotrophic hypogonadism, elevated estrogen level, and malnutrition all contribute to the problem.1 However, most premenopausal women experience a return of their menstrual cycle, and possibly of fertility, within the first 10 months after liver transplant,2,3 after which pregnancy is possible.

In transplant recipients of childbearing age, the need for preconception counseling and family planning should be emphasized. The timing, potential risks, and outcomes of pregnancy, and the importance of coordinated prenatal and perinatal care should be addressed.4 The National Transplant Pregnancy Registry guidelines recommend postponing conception until:

  • At least 1 year has elapsed after transplant
  • Graft function is stable
  • Medical comorbidities such as diabetes and hypertension are well controlled
  • Immunosuppression is at a low maintenance level.3

Strong evidence suggests that an appropriate liver transplant-conception interval reduces adverse maternal and fetal outcomes. In particular, the risks of a low birth weight, graft rejection, and loss during pregnancy are significantly decreased.3 Therefore, contraception must be initiated after transplant before any sexual activity, with no preference as to the form of protection used.

Limited data demonstrate the safety and efficacy of combined oral contraceptives and transdermal contraceptive patches in stable solid-organ recipients.5,6 Estrogen-containing contraceptives should, however, be avoided in recurrent liver disease after transplant because of the risk of increased hepatic toxicity.

MANAGING RISKS ASSOCIATED WITH PREGNANCY

Physicians should be alert to the possibility of a pregnancy. Early diagnosis allows the optimization of management and outcomes, as complications are increased in this population of expectant mothers.7

Well-known risks to the expectant liver transplant recipient include hypertension and preeclampsia.8 Moreover, infants born to these patients have a higher risk of prematurity and low birth weight.3,7,9 However, rates of neonatal or maternal deaths and birth defects do not differ significantly from those seen in the general population. Graft rejection is a potential complication, with rates varying between 0% and 20% in different studies.3

Multidisciplinary care is therefore crucial during these high-risk pregnancies.10 An obstetrician, a hepatologist, and a perinatalogist should collaborate to maximize outcomes.11 Frequent evaluations, preferably 2 weeks apart, are suggested for the serial assessment of fetal growth.

Furthermore, daily monitoring of the blood pressure and aggressive management of hypertension are recommended. Methyldopa appears to be the drug treatment of choice.12

Close monitoring of graft function and liver biopsy in suspected graft rejection are of essence as well.3 Routine screening for urinary tract infection, cytomegalovirus and toxoplasmosis infections, gestational diabetes, and preeclampsia should also be undertaken.

MANAGING IMMUNOSUPPRESSION IN THE PREGNANT PATIENT

The choice of immunosuppression is ideally made before pregnancy. All immunosuppressive drugs cross the placenta. Thus, in theory, all agents carry risks of teratogenicity and fetal loss. However, immunosuppression is crucial in avoiding rejection. Furthermore, the use of appropriate immunosuppressive regimens prevents negative outcomes. Drugs are classified as class A (safest to use in pregnancy), through classes B, C, D, and X.

Tacrolimus (class C) monotherapy appears to be safe, with attention to the maintenance of therapeutic levels throughout pregnancy. Allograft function and tacrolimus serum levels need to be monitored because of the change in the volume of drug distribution. Cyclosporine (a pregnancy class C drug), prednisone (class B), and azathioprine (class D) are also reasonable options and may also be used if judged necessary.13

Mycophenolic acid and mTOR (mammalian target of rapamycin) inhibitors such as sirolimus and everolimus are significantly teratogenic and should be avoided in pregnant women. They are more commonly associated with spontaneous abortion, structural abnormalities, and birth defects than other immunosuppressive drugs, especially if taken in the early stages of pregnancy. Cleft lip and palate, absent auditory canals, and microtia have been reported.2,13

References
  1. Bell H, Raknerud N, Falch JA, Haug E. Inappropriately low levels of gonadotrophins in amenorrhoeic women with alcoholic and non-alcoholic cirrhosis. Eur J Endocrinol 1995; 132:444–449.
  2. Mass K, Quint EH, Punch MR, Merion RM. Gynecological and reproductive function after liver transplantation. Transplantation 1996; 62:476–479.
  3. Coscia LA, Constantinescu S, Moritz MJ, et al. Report from the National Transplantation Pregnancy Registry (NTPR): outcomes of pregnancy after transplantation. Clin Transpl 2009; 103–122.
  4. Parolin MB, Coelho JC, Urbanetz AA, Pampuch M. Contraception and pregnancy after liver transplantation: an update overview. Arq Gastroenterol 2009; 46:154–158. In Portuguese.
  5. Paulen ME, Folger SG, Curtis KM, Jamieson DJ. Contraceptive use among solid organ transplant patients: a systematic review. Contraception 2010; 82:102–112.
  6. Jabiry-Zieniewicz Z, Bobrowska K, Kaminski P, Wielgos M, Zieniewicz K, Krawczyk M. Low-dose hormonal contraception after liver transplantation. Transplant Proc 2007; 39:1530–1532.
  7. Coffin CS, Shaheen AA, Burak KW, Myers RP. Pregnancy outcomes among liver transplant recipients in the United States: a nationwide case-control analysis. Liver Transpl 2010; 16:56–63.
  8. Heneghan MA, Selzner M, Yoshida EM, Mullhaupt B. Pregnancy and sexual function in liver transplantation. J Hepatol 2008; 49:507–519.
  9. Ho JK, Ko HH, Schaeffer DF, et al. Sexual health after orthotopic liver transplantation. Liver Transpl 2006; 12:1478–1484.
  10. Jabiry-Zieniewicz Z, Dabrowski FA, Pietrzak B, Wielgos M. Pregnancy complications after liver transplantation. Int J Gynaecol Obstet 2015; 128:27–29.
  11. Parhar KS, Gibson PS, Coffin CS. Pregnancy following liver transplantation: review of outcomes and recommendations for management. Can J Gastroenterol 2012; 26:621–626.
  12. McKay DB, Josephson MA, Armenti VT, et al; Women’s Health Committee of the American Society of Transplantation. Reproduction and transplantation: report on the AST Consensus Conference on Reproductive Issues and Transplantation. Am J Transplant 2005; 5:1592–1599.
  13. Sifontis NM, Coscia LA, Constantinescu S, Lavelanet AF, Moritz MJ, Armenti VT. Pregnancy outcomes in solid organ transplant recipients with exposure to mycophenolate mofetil or sirolimus. Transplantation 2006; 82:1698–1702.
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Chelala_PregnancyAndLiverTransplant.pdf
Author and Disclosure Information

Lydia Chelala, MD
Department of Internal Medicine, Staten Island University Hospital, New York, NY

Ghassan Ilaiwy, MD
Department of Internal Medicine, Medstar Washington Hospital Center, Washington, DC

Ibrahim A. Hanouneh, MD
Minnesota Gastroenterology, P.A., Minneapolis, MN

Address: Ibrahim A. Hanouneh, MD, Minnesota Gastroenterology, P.A., P.O. Box 14909, Minneapolis, MN 55414; ibrahimhanouneh@gmail.com

Issue
Cleveland Clinic Journal of Medicine - 83(7)
Publications
Cleveland Clinic Journal of Medicine
Topics
Hepatology
Women's Health
Page Number
498-499
Legacy Keywords
Liver transplant, pregnant, fertility, immunosuppression Lydia Chelala, Ghassan Ilaiwy, Ibrahim Hanouneh
Sections
1-Minute Consult
Author(s)
Lydia Chelala, MD
Ghassan Ilaiwy, MD
Ibrahim A. Hanouneh, MD
Author(s)
Lydia Chelala, MD
Ghassan Ilaiwy, MD
Ibrahim A. Hanouneh, MD
Author and Disclosure Information

Lydia Chelala, MD
Department of Internal Medicine, Staten Island University Hospital, New York, NY

Ghassan Ilaiwy, MD
Department of Internal Medicine, Medstar Washington Hospital Center, Washington, DC

Ibrahim A. Hanouneh, MD
Minnesota Gastroenterology, P.A., Minneapolis, MN

Address: Ibrahim A. Hanouneh, MD, Minnesota Gastroenterology, P.A., P.O. Box 14909, Minneapolis, MN 55414; ibrahimhanouneh@gmail.com

Author and Disclosure Information

Lydia Chelala, MD
Department of Internal Medicine, Staten Island University Hospital, New York, NY

Ghassan Ilaiwy, MD
Department of Internal Medicine, Medstar Washington Hospital Center, Washington, DC

Ibrahim A. Hanouneh, MD
Minnesota Gastroenterology, P.A., Minneapolis, MN

Address: Ibrahim A. Hanouneh, MD, Minnesota Gastroenterology, P.A., P.O. Box 14909, Minneapolis, MN 55414; ibrahimhanouneh@gmail.com

Article PDF
Chelala_PregnancyAndLiverTransplant.pdf
Article PDF
Chelala_PregnancyAndLiverTransplant.pdf
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Yes, pregnancy is possible, but not immediately after transplant, and it involves risks. Appropriate management and multidisciplinary care are necessary to optimize the outcomes.

HOW LONG SHOULD PREGNANCY BE POSTPONED?

Hypogonadism and amenorrhea are common and multifactorial in women with end-stage liver disease. Hypogonadotrophic hypogonadism, elevated estrogen level, and malnutrition all contribute to the problem.1 However, most premenopausal women experience a return of their menstrual cycle, and possibly of fertility, within the first 10 months after liver transplant,2,3 after which pregnancy is possible.

In transplant recipients of childbearing age, the need for preconception counseling and family planning should be emphasized. The timing, potential risks, and outcomes of pregnancy, and the importance of coordinated prenatal and perinatal care should be addressed.4 The National Transplant Pregnancy Registry guidelines recommend postponing conception until:

  • At least 1 year has elapsed after transplant
  • Graft function is stable
  • Medical comorbidities such as diabetes and hypertension are well controlled
  • Immunosuppression is at a low maintenance level.3

Strong evidence suggests that an appropriate liver transplant-conception interval reduces adverse maternal and fetal outcomes. In particular, the risks of a low birth weight, graft rejection, and loss during pregnancy are significantly decreased.3 Therefore, contraception must be initiated after transplant before any sexual activity, with no preference as to the form of protection used.

Limited data demonstrate the safety and efficacy of combined oral contraceptives and transdermal contraceptive patches in stable solid-organ recipients.5,6 Estrogen-containing contraceptives should, however, be avoided in recurrent liver disease after transplant because of the risk of increased hepatic toxicity.

MANAGING RISKS ASSOCIATED WITH PREGNANCY

Physicians should be alert to the possibility of a pregnancy. Early diagnosis allows the optimization of management and outcomes, as complications are increased in this population of expectant mothers.7

Well-known risks to the expectant liver transplant recipient include hypertension and preeclampsia.8 Moreover, infants born to these patients have a higher risk of prematurity and low birth weight.3,7,9 However, rates of neonatal or maternal deaths and birth defects do not differ significantly from those seen in the general population. Graft rejection is a potential complication, with rates varying between 0% and 20% in different studies.3

Multidisciplinary care is therefore crucial during these high-risk pregnancies.10 An obstetrician, a hepatologist, and a perinatalogist should collaborate to maximize outcomes.11 Frequent evaluations, preferably 2 weeks apart, are suggested for the serial assessment of fetal growth.

Furthermore, daily monitoring of the blood pressure and aggressive management of hypertension are recommended. Methyldopa appears to be the drug treatment of choice.12

Close monitoring of graft function and liver biopsy in suspected graft rejection are of essence as well.3 Routine screening for urinary tract infection, cytomegalovirus and toxoplasmosis infections, gestational diabetes, and preeclampsia should also be undertaken.

MANAGING IMMUNOSUPPRESSION IN THE PREGNANT PATIENT

The choice of immunosuppression is ideally made before pregnancy. All immunosuppressive drugs cross the placenta. Thus, in theory, all agents carry risks of teratogenicity and fetal loss. However, immunosuppression is crucial in avoiding rejection. Furthermore, the use of appropriate immunosuppressive regimens prevents negative outcomes. Drugs are classified as class A (safest to use in pregnancy), through classes B, C, D, and X.

Tacrolimus (class C) monotherapy appears to be safe, with attention to the maintenance of therapeutic levels throughout pregnancy. Allograft function and tacrolimus serum levels need to be monitored because of the change in the volume of drug distribution. Cyclosporine (a pregnancy class C drug), prednisone (class B), and azathioprine (class D) are also reasonable options and may also be used if judged necessary.13

Mycophenolic acid and mTOR (mammalian target of rapamycin) inhibitors such as sirolimus and everolimus are significantly teratogenic and should be avoided in pregnant women. They are more commonly associated with spontaneous abortion, structural abnormalities, and birth defects than other immunosuppressive drugs, especially if taken in the early stages of pregnancy. Cleft lip and palate, absent auditory canals, and microtia have been reported.2,13

Yes, pregnancy is possible, but not immediately after transplant, and it involves risks. Appropriate management and multidisciplinary care are necessary to optimize the outcomes.

HOW LONG SHOULD PREGNANCY BE POSTPONED?

Hypogonadism and amenorrhea are common and multifactorial in women with end-stage liver disease. Hypogonadotrophic hypogonadism, elevated estrogen level, and malnutrition all contribute to the problem.1 However, most premenopausal women experience a return of their menstrual cycle, and possibly of fertility, within the first 10 months after liver transplant,2,3 after which pregnancy is possible.

In transplant recipients of childbearing age, the need for preconception counseling and family planning should be emphasized. The timing, potential risks, and outcomes of pregnancy, and the importance of coordinated prenatal and perinatal care should be addressed.4 The National Transplant Pregnancy Registry guidelines recommend postponing conception until:

  • At least 1 year has elapsed after transplant
  • Graft function is stable
  • Medical comorbidities such as diabetes and hypertension are well controlled
  • Immunosuppression is at a low maintenance level.3

Strong evidence suggests that an appropriate liver transplant-conception interval reduces adverse maternal and fetal outcomes. In particular, the risks of a low birth weight, graft rejection, and loss during pregnancy are significantly decreased.3 Therefore, contraception must be initiated after transplant before any sexual activity, with no preference as to the form of protection used.

Limited data demonstrate the safety and efficacy of combined oral contraceptives and transdermal contraceptive patches in stable solid-organ recipients.5,6 Estrogen-containing contraceptives should, however, be avoided in recurrent liver disease after transplant because of the risk of increased hepatic toxicity.

MANAGING RISKS ASSOCIATED WITH PREGNANCY

Physicians should be alert to the possibility of a pregnancy. Early diagnosis allows the optimization of management and outcomes, as complications are increased in this population of expectant mothers.7

Well-known risks to the expectant liver transplant recipient include hypertension and preeclampsia.8 Moreover, infants born to these patients have a higher risk of prematurity and low birth weight.3,7,9 However, rates of neonatal or maternal deaths and birth defects do not differ significantly from those seen in the general population. Graft rejection is a potential complication, with rates varying between 0% and 20% in different studies.3

Multidisciplinary care is therefore crucial during these high-risk pregnancies.10 An obstetrician, a hepatologist, and a perinatalogist should collaborate to maximize outcomes.11 Frequent evaluations, preferably 2 weeks apart, are suggested for the serial assessment of fetal growth.

Furthermore, daily monitoring of the blood pressure and aggressive management of hypertension are recommended. Methyldopa appears to be the drug treatment of choice.12

Close monitoring of graft function and liver biopsy in suspected graft rejection are of essence as well.3 Routine screening for urinary tract infection, cytomegalovirus and toxoplasmosis infections, gestational diabetes, and preeclampsia should also be undertaken.

MANAGING IMMUNOSUPPRESSION IN THE PREGNANT PATIENT

The choice of immunosuppression is ideally made before pregnancy. All immunosuppressive drugs cross the placenta. Thus, in theory, all agents carry risks of teratogenicity and fetal loss. However, immunosuppression is crucial in avoiding rejection. Furthermore, the use of appropriate immunosuppressive regimens prevents negative outcomes. Drugs are classified as class A (safest to use in pregnancy), through classes B, C, D, and X.

Tacrolimus (class C) monotherapy appears to be safe, with attention to the maintenance of therapeutic levels throughout pregnancy. Allograft function and tacrolimus serum levels need to be monitored because of the change in the volume of drug distribution. Cyclosporine (a pregnancy class C drug), prednisone (class B), and azathioprine (class D) are also reasonable options and may also be used if judged necessary.13

Mycophenolic acid and mTOR (mammalian target of rapamycin) inhibitors such as sirolimus and everolimus are significantly teratogenic and should be avoided in pregnant women. They are more commonly associated with spontaneous abortion, structural abnormalities, and birth defects than other immunosuppressive drugs, especially if taken in the early stages of pregnancy. Cleft lip and palate, absent auditory canals, and microtia have been reported.2,13

References
  1. Bell H, Raknerud N, Falch JA, Haug E. Inappropriately low levels of gonadotrophins in amenorrhoeic women with alcoholic and non-alcoholic cirrhosis. Eur J Endocrinol 1995; 132:444–449.
  2. Mass K, Quint EH, Punch MR, Merion RM. Gynecological and reproductive function after liver transplantation. Transplantation 1996; 62:476–479.
  3. Coscia LA, Constantinescu S, Moritz MJ, et al. Report from the National Transplantation Pregnancy Registry (NTPR): outcomes of pregnancy after transplantation. Clin Transpl 2009; 103–122.
  4. Parolin MB, Coelho JC, Urbanetz AA, Pampuch M. Contraception and pregnancy after liver transplantation: an update overview. Arq Gastroenterol 2009; 46:154–158. In Portuguese.
  5. Paulen ME, Folger SG, Curtis KM, Jamieson DJ. Contraceptive use among solid organ transplant patients: a systematic review. Contraception 2010; 82:102–112.
  6. Jabiry-Zieniewicz Z, Bobrowska K, Kaminski P, Wielgos M, Zieniewicz K, Krawczyk M. Low-dose hormonal contraception after liver transplantation. Transplant Proc 2007; 39:1530–1532.
  7. Coffin CS, Shaheen AA, Burak KW, Myers RP. Pregnancy outcomes among liver transplant recipients in the United States: a nationwide case-control analysis. Liver Transpl 2010; 16:56–63.
  8. Heneghan MA, Selzner M, Yoshida EM, Mullhaupt B. Pregnancy and sexual function in liver transplantation. J Hepatol 2008; 49:507–519.
  9. Ho JK, Ko HH, Schaeffer DF, et al. Sexual health after orthotopic liver transplantation. Liver Transpl 2006; 12:1478–1484.
  10. Jabiry-Zieniewicz Z, Dabrowski FA, Pietrzak B, Wielgos M. Pregnancy complications after liver transplantation. Int J Gynaecol Obstet 2015; 128:27–29.
  11. Parhar KS, Gibson PS, Coffin CS. Pregnancy following liver transplantation: review of outcomes and recommendations for management. Can J Gastroenterol 2012; 26:621–626.
  12. McKay DB, Josephson MA, Armenti VT, et al; Women’s Health Committee of the American Society of Transplantation. Reproduction and transplantation: report on the AST Consensus Conference on Reproductive Issues and Transplantation. Am J Transplant 2005; 5:1592–1599.
  13. Sifontis NM, Coscia LA, Constantinescu S, Lavelanet AF, Moritz MJ, Armenti VT. Pregnancy outcomes in solid organ transplant recipients with exposure to mycophenolate mofetil or sirolimus. Transplantation 2006; 82:1698–1702.
References
  1. Bell H, Raknerud N, Falch JA, Haug E. Inappropriately low levels of gonadotrophins in amenorrhoeic women with alcoholic and non-alcoholic cirrhosis. Eur J Endocrinol 1995; 132:444–449.
  2. Mass K, Quint EH, Punch MR, Merion RM. Gynecological and reproductive function after liver transplantation. Transplantation 1996; 62:476–479.
  3. Coscia LA, Constantinescu S, Moritz MJ, et al. Report from the National Transplantation Pregnancy Registry (NTPR): outcomes of pregnancy after transplantation. Clin Transpl 2009; 103–122.
  4. Parolin MB, Coelho JC, Urbanetz AA, Pampuch M. Contraception and pregnancy after liver transplantation: an update overview. Arq Gastroenterol 2009; 46:154–158. In Portuguese.
  5. Paulen ME, Folger SG, Curtis KM, Jamieson DJ. Contraceptive use among solid organ transplant patients: a systematic review. Contraception 2010; 82:102–112.
  6. Jabiry-Zieniewicz Z, Bobrowska K, Kaminski P, Wielgos M, Zieniewicz K, Krawczyk M. Low-dose hormonal contraception after liver transplantation. Transplant Proc 2007; 39:1530–1532.
  7. Coffin CS, Shaheen AA, Burak KW, Myers RP. Pregnancy outcomes among liver transplant recipients in the United States: a nationwide case-control analysis. Liver Transpl 2010; 16:56–63.
  8. Heneghan MA, Selzner M, Yoshida EM, Mullhaupt B. Pregnancy and sexual function in liver transplantation. J Hepatol 2008; 49:507–519.
  9. Ho JK, Ko HH, Schaeffer DF, et al. Sexual health after orthotopic liver transplantation. Liver Transpl 2006; 12:1478–1484.
  10. Jabiry-Zieniewicz Z, Dabrowski FA, Pietrzak B, Wielgos M. Pregnancy complications after liver transplantation. Int J Gynaecol Obstet 2015; 128:27–29.
  11. Parhar KS, Gibson PS, Coffin CS. Pregnancy following liver transplantation: review of outcomes and recommendations for management. Can J Gastroenterol 2012; 26:621–626.
  12. McKay DB, Josephson MA, Armenti VT, et al; Women’s Health Committee of the American Society of Transplantation. Reproduction and transplantation: report on the AST Consensus Conference on Reproductive Issues and Transplantation. Am J Transplant 2005; 5:1592–1599.
  13. Sifontis NM, Coscia LA, Constantinescu S, Lavelanet AF, Moritz MJ, Armenti VT. Pregnancy outcomes in solid organ transplant recipients with exposure to mycophenolate mofetil or sirolimus. Transplantation 2006; 82:1698–1702.
Issue
Cleveland Clinic Journal of Medicine - 83(7)
Issue
Cleveland Clinic Journal of Medicine - 83(7)
Page Number
498-499
Page Number
498-499
Publications
Cleveland Clinic Journal of Medicine
Publications
Cleveland Clinic Journal of Medicine
Topics
Hepatology
Women's Health
Article Type
Article
Display Headline
A female liver transplant recipient asks: Can I become pregnant?
Display Headline
A female liver transplant recipient asks: Can I become pregnant?
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Liver transplant, pregnant, fertility, immunosuppression Lydia Chelala, Ghassan Ilaiwy, Ibrahim Hanouneh
Legacy Keywords
Liver transplant, pregnant, fertility, immunosuppression Lydia Chelala, Ghassan Ilaiwy, Ibrahim Hanouneh
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