Serum Alanine Aminotransferase and Hepatitis B DNA Flares in Pregnant and Postpartum Women with Chronic Hepatitis B

Chang, C. Y.; Aziz, Najib; Poongkunran, Mugilan; Javaid, Asad; Trinh, Huy N.; Lau, Daryl; Nguyen, Mindie H.

doi:10.1038/ajg.2016.296

Cited by 72 publications

(81 citation statements)

References 32 publications

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“…HBV flares during pregnancy are infrequent. In a longitudinal study of US women who were not on antiviral therapy pre-pregnancy, only 6% experienced a ≥2-log increase in HBV DNA during pregnancy accompanied by ALT flares [6]. For women on antiviral therapy pre-pregnancy who stop treatment when pregnancy is diagnosed, viral rebound with ALT flare appears to occur more frequently (67% in one study) followed by spontaneous recovery in the vast majority [7].…”

Section: Hbv and Pregnancymentioning

confidence: 99%

“…The majority of flares were subclinical – although there are rare reports of hepatic decompensation, likely in women who had advanced fibrosis during pregnancy. Whether HBV DNA levels predict risk of flares is unclear [6,10]. The frequency of flares in women who stopped antivirals at or soon after delivery appears similar or slightly higher than women not treated with antivirals during pregnancy [11].…”

Section: Hbv and Pregnancymentioning

confidence: 99%

“…The frequency of flares in women who stopped antivirals at or soon after delivery appears similar or slightly higher than women not treated with antivirals during pregnancy [11]. Continuation of antiviral therapy post-partum does not prevent flares [6,11] and most flares resolve without intervention.…”

Section: Hbv and Pregnancymentioning

confidence: 99%

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Management of hepatitis B in special populations

Zhou

Terrault

2017

Best Practice & Research Clinical Gastroenterology

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Special populations infected with chronic HBV include those with decompensated cirrhosis, coinfections (HIV, HCV, HDV), hemodialysis and renal failure, immunosuppressed including transplant patients, children and women in pregnancy. These populations differ in their natural history and risk for liver-related complications, the indications for anti-HBV therapy as well as the recommendations regarding the HBV drugs used, duration of therapy and anticipated endpoints. Reflecting the special populations with substantive changes in management in recent years, this review focuses on HBV-HIV coinfected patients, immunosuppressed patients at risk for reactivation, liver transplant recipients and pregnant women. Management of women in the context of pregnancy and post-partum requires consideration of risks to mother and fetus/infant, including the risk of mother-to-child transmission. HBV-HIV coinfected patients require initiation of treatment concurrent with their HIV therapy and the HBV drugs used must by selected to minimize HIV and HBV resistance long-term. Increasing recognition of the risk for HBV reactivation with immunosuppressive therapy has led to recommendations to use prophylactic HBV therapy in patients with moderate to high risk of reactivation. Liver transplant recipients with HBV require life-long therapy to prevent or treat HBV infection but with current therapies, graft and patient survival are excellent.

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Section: Hbv and Pregnancymentioning

confidence: 99%

Section: Hbv and Pregnancymentioning

confidence: 99%

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Management of hepatitis B in special populations

Zhou

Terrault

2017

Best Practice & Research Clinical Gastroenterology

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“…However, restoration of the CMI function occurs during the postpartum period, and studies have reported higher than expected HBeAg seroconversion rates [24] and higher than normal rates of alanine aminotransferase (ALT) during the initial postpartum period in HBVinfected women [23,[25][26][27][28][29]. While most hepatic flares have been mild and resolved spontaneously [25], a small number of case reports indicate severe hepatitis flares leading to hepatic decompensation during the peripartum period [29]. Some experts have suggested that HBV DNA and ALT should be monitored every 4-6 weeks during the first and second trimesters, every 4 weeks during the third trimester, and at postpartum months 3 and 6 in women with CHB [29].…”

Section: Effects Of Pregnancy On Hbv-associated Liver Diseasementioning

confidence: 99%

“…While most hepatic flares have been mild and resolved spontaneously [25], a small number of case reports indicate severe hepatitis flares leading to hepatic decompensation during the peripartum period [29]. Some experts have suggested that HBV DNA and ALT should be monitored every 4-6 weeks during the first and second trimesters, every 4 weeks during the third trimester, and at postpartum months 3 and 6 in women with CHB [29]. The APASL recommends checking maternal HBeAg, HBV DNA status, and ALT levels during pregnancy to determine liver disease activity and the risk of MTCT [14].…”

Section: Effects Of Pregnancy On Hbv-associated Liver Diseasementioning

confidence: 99%

Hepatitis B During Pregnancy in Endemic Areas: Screening, Treatment, and Prevention of Mother-to-Child Transmission

Chamroonkul

Piratvisuth

2017

Pediatr Drugs

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The proper management of pregnant women infected with hepatitis B virus (HBV) is necessary to prevent maternal and fetal morbidity and mortality and to protect the baby from HBV infection. In the majority of cases, vertical transmission can be prevented with a universal screening program, HBV vaccine immunoprophylaxis, and administration of hepatitis B immunoglobulin (HBIg) for babies born to mothers with HBV. However, in mothers with a high viral load (>200,000 or >1,000,000 IU/ml, depending on the guideline), the chance of immunoprophylaxis failure remains high. The standard recommendation is to give an antiviral agent during the third trimester in these patients. US FDA pregnancy category B agents such as tenofovir and telbivudine are allowed through all trimesters of pregnancy. Breastfeeding for patients who receive antiviral agents can be allowed after a risk-benefit discussion with the patient.

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The management of hepatitis B virus in pregnancy

Chan

2020

Clinical Dilemmas in Viral Liver Disease

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Serum Alanine Aminotransferase and Hepatitis B DNA Flares in Pregnant and Postpartum Women with Chronic Hepatitis B

Abstract: Flares in HBV DNA and ALT can occur during late pregnancy and early postpartum in CHB women, and can be severe. Women with CHB should therefore be closely monitored during pregnancy and early postpartum.

Cited by 72 publications

References 32 publications

Management of hepatitis B in special populations

Management of hepatitis B in special populations

Hepatitis B During Pregnancy in Endemic Areas: Screening, Treatment, and Prevention of Mother-to-Child Transmission

The management of hepatitis B virus in pregnancy

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