Ten-year neonatal hepatitis B vaccination program, the Netherlands, 1982–1992: protective efficacy and long-term immunogenicity

doi:10.1016/S0264-410X(97)00080-7

Vaccine

Volume 15, Issue 15, October 1997, Pages 1624-1630

https://doi.org/10.1016/S0264-410X(97)00080-7 Get rights and content

Abstract

From 1982 to 1989, 705 infants born to HBsAg-positive mothers entered the Dutch neonatal hepatitis B vaccination program and received passive-active hepatitis B immunization in three randomized controlled trials testing variations in time of starting active vaccination, dose and type of vaccine, and number of hepatitis B immunoglobulin (HBIg) injections. A meta-analysis of individual patient data of the three randomized trials was performed to determine which independent host and vaccination related factors influence protective efficacy and long-term immunogenicity, and to assess whether hepatitis B vaccination concomitant with standard DKTP vaccination provides optimal protection. Statistical methodology included multivariate logistic regression analysis. Eight infants (1.1%), all born to HBeAg-positive mothers, became HBsAg carriers within the first year of life. The protective efficacy rate (PER) of passive-active immunization at 12 months follow-up was 92% for the total group of children from 114 HBeAg-positive mothers with no significant differences between children starting active immunization at birth or at 3 months of age, between infants starting at 3 months of age receiving one or two doses of HBIg or between those receiving plasma derived or recombinant vaccine. The only factor that affected the PER significantly was the level of maternal HBV DNA; PER was 100% if maternal HBV DNA was <150 pg ml⁻¹ and 68% for HBV DNA levels > 150 pg ml⁻¹. After 5 years of follow-up, the group that started active immunization at birth had significantly more infants with loss of seroprotection (anti-HBs levels < 10 IU l⁻¹, 15%) than the corresponding group starting at 3 months of age (anti-HBs < 10 IU l⁻², 2%). One of 35 children with loss of seroprotection at 2 years became a HBsAg carrier in the fifth year of follow-up. This meta-analysis shows that the protective efficacy of passive-active hepatitis B vaccination is mainly influenced by material HBV DNA levels, and independent of the time of starting active vaccination at birth or at 3 monts of age; long-term immunity was enhanced by starting active vaccination concomitant with DKTP vaccination. These findings allow incorporation of hepatitis B vaccine into the standard infant immunization programs for countries with a passive-active immunization strategy for the control of hepatitis B. Additional measures are needed to protect neonates of highly viremic women.

References (22)

P.M. Grosheide et al.
Anti-HBs levels in infants of hepatitis B carrier mothers after delayed active immunization with recombinant vaccine concomitant with DTP-Polio vaccine: Is there need for a second dose of HBlg?
Vaccine
(1994)
R. del Canho et al.
Failure of neonatal hepatitis B vaccination: The role of HBV DNA levels in hepatitis B carrier mothers and HLA antigens in neonates
Journal of Hepatology
(1994)
H.M.H. Ip et al.
Prevention of hepatitis B virus carrier state in infants according to maternal serum levels of HBV DNA
Lancet
(1989)
H.H. Lin et al.
Early predictor of the efficacy of immunoprophylaxis against perinatal hepatitis B transmission: analysis of prophylaxis failure
Vaccine
(1991)
R.P. Beasley et al.
Prevention of perinatally transmitted hepatitis B virus infections with hepatitis B immune globulin and hepatitis B vaccine
Lancet
(1983)
V.C.W. Wong et al.
Prevention of the HBsAg carrier state in newborn infants of mothers who are chronic carriers of HBsAg and HBeAg by administration of hepatitis B vaccine and hepatitis B immunoglobulin
Lancet
(1984)
P. Coursaget et al.
Seven-year study of hepatitis B vaccine efficacy in infants from an endemic area (Senegal)
Lancet
(1986)
W.F. Carman et al.
Vaccine-induced escape mutant of hepatitis B virus
Lancet
(1990)
J.A. Mazel et al.
Passive-active immunisation of neonates of HBsAg positive carrier mothers: preliminary observations
British Medical Journal
(1984)
S.W. Schalm et al.
Prevention of hepatitis B infection in newborns through mass screening and delayed vaccination of all infants of mothers with hepatitis B surface antigen
Pediatrics
(1989)

S.D. Lee et al.

Prevention of maternal-infant hepatitis B virus transmission by immunization: The role of serum hepatitis B virus DNA

Hepatology

(1986)

Cited by (173)

Society for Maternal-Fetal Medicine Consult Series #69: Hepatitis B in pregnancy: updated guidelines
2024, American Journal of Obstetrics and Gynecology
More than 290 million people worldwide, and almost 2 million people in the United States, are infected with hepatitis B virus, which can lead to chronic hepatitis B, a vaccine-preventable communicable disease. The prevalence of chronic hepatitis B infection in pregnancy is estimated to be 0.7% to 0.9% in the United States, with >25,000 infants born annually at risk for chronic infection due to perinatal transmission. Given the burden of disease associated with chronic hepatitis B infection, recent national guidance has expanded both the indications for screening for hepatitis B infection and immunity and the indications for vaccination. The purpose of this document is to aid clinicians caring for pregnant patients in screening for hepatitis B infection and immunity status, discuss the perinatal risks of hepatitis B infection in pregnancy, determine whether treatment is indicated for maternal or perinatal indications, and recommend hepatitis B vaccination among susceptible patients. The following are the Society for Maternal-Fetal Medicine recommendations: (1) we recommend triple-panel testing (hepatitis B surface antigen screening, antibody to hepatitis B surface antigen, and total antibody to hepatitis B core antigen) at the initial prenatal visit if not previously documented or known to have been performed (GRADE 1C); (2) we recommend universal hepatitis B surface antigen screening alone at the initial prenatal care visit for all pregnancies where there has been a previously documented negative triple-panel test (GRADE 1B); (3) we recommend that individuals with unknown hepatitis B surface antigen screening status be tested on any presentation for care in pregnancy; we also recommend that those with clinical hepatitis or those with risk factors for acute hepatitis B infection be tested at the time of admission to a birthing facility when delivery is anticipated (GRADE 1B); (4) we do not recommend altering routine intrapartum care in individuals chronically infected with hepatitis B; administration of neonatal immunoprophylaxis is standard of care in these situations (GRADE 1B); (5) we do not recommend cesarean delivery for the sole indication of reducing perinatal hepatitis B virus transmission (GRADE 1B); (6) we recommend that individuals with HBV infection can breastfeed as long as the infant has received immunoprophylaxis at birth (GRADE 1C); (7) we suggest individuals with hepatitis B infection who desire invasive testing may have the procedure performed after an informed discussion on risks and benefits in the context of shared decision-making and in the context of how testing will affect clinical care (GRADE 2C); (8) in individuals with hepatitis viral loads >200,000 IU/mL (>5.3 log 10 IU/mL), we recommend antiretroviral therapy with tenofovir (tenofovir alafenamide at 25 mg daily or tenofovir disoproxil fumarate at 300 mg daily) in the third trimester (initiated at 28–32 weeks of gestation) as an adjunctive strategy to immunoprophylaxis to reduce perinatal transmission (GRADE 1B); (9) we recommend administering hepatitis B vaccine and hepatitis B immunoglobin within 12 hours of birth to all newborns of hepatitis B surface antigen–positive pregnant patients or those with unknown or undocumented hepatitis B surface antigen status, regardless of whether antiviral therapy has been given during the pregnancy to the pregnant patient (GRADE 1B); and (10) we recommend hepatitis B vaccination in pregnancy for all individuals without serologic evidence of immunity or documented history of vaccination (GRADE 1C).
Management of Viral Complications of Pregnancy: Pharmacotherapy to Reduce Vertical Transmission
2021, Obstetrics and Gynecology Clinics of North America
Maternal HBeAg positivity and viremia associated with umbilical cord blood hepatitis B viremia
2019, Pediatrics and Neonatology
Hepatitis B (HBV) transmission may result from in utero transmission. We aimed to determine the correlation between maternal serum and umbilical cord blood HBV DNA levels in infants delivered by chronic HBV-infected mothers and to describe the effect of cord blood viremia on vertical transmission.
A prospective cohort of 92 chronic HBV-infected mother-and-child pairs recruited over three years was analyzed. Maternal and cord blood were tested for HBV DNA by real-time PCR. Standard immunoprophylaxis with both active and passive immunization was administered to all infants. Serological testing was performed on all infants at 9 months of age.
Moderate positive correlation of the maternal HBV DNA with cord blood HBV DNA was demonstrated (r² = 0.521, p = <0.001). HBeAg +ve mothers were younger with higher HBV and cord viremia. At 9 months of age, one infant was infected. Infants delivered by HBeAg positive mothers and mothers with high HBV DNA of more than 6 LOG IU/mL (1 x 10⁶ IU/mL) have increased relative risk of cord blood viremia.
Maternal HBV DNA and presence of HBeAg were positively correlated to cord blood HBV DNA in infants delivered by chronic HBV-infected mothers. Our data suggest that reducing maternal viremia during the antenatal period may help to reduce cord blood viremia.
Treatment of Viral Infections During Pregnancy
2019, Clinics in Perinatology
Clinical course and perinatal transmission of chronic hepatitis B during pregnancy: A real-world prospective cohort study
2017, Journal of Infection
Citation Excerpt :
There is limited data on perinatal transmission rates in CHB patients with low HBV-DNA levels. One previous study reported that perinatal transmission only occurred when the mothers' HBV-DNA levels were as high as >150 pg/mL (equivalent to around 4 × 107 copies/mL).19 Children born to HBeAg-negative mothers seemed to be at quite low risk (<1%) for chronic HBV infection after the immunoprophylaxis program.1,20
To determine the clinical course and perinatal transmission of chronic hepatitis B during pregnancy in a real life setting.
A total of 221 singleton pregnant women with detectable HBV-DNA levels (≥10³ copies/mL) were enrolled during January 2011 to June 2015. Forty-three high viraemic patients (≥10⁶ copies/mL) received telbivudine in the 2^nd or 3^rd trimester according to their intention, while 89 high viraemic and 79 low viraemic (≥10³ and <10⁶ copies/mL) patients were the control cohorts. Primary endpoint was the pregnancy outcomes and secondary endpoint the perinatal transmission including intrauterine infection, immunoprophylaxis failure and occult infection.
In all, 209 patients completed pregnancy with 209 infants, while 2 in telbivudine-treated cohort had unexplained late stillbirths. Twenty-nine (70.7%) of telbivudine-treated patients and 3 (3.4%) of untreated high viraemic controls achieved undetectable HBV-DNA levels prior delivery. At 7 months postpartum, immunoprophylaxis failure was significantly lower (2.4%) in telbivudine-treated cohort, compared with 16.9% and 10.1% in untreated high and low viraemic cohorts, respectively.
Low viraemic patients may also need antiviral therapy since they bear moderate risk for perinatal transmission of HBV. However, more multicenter, large-scale studies are required before antepartum antiviral therapy is routinely recommended in patients with detectable viral loads.
Hepatitis B Vaccines
2017, Plotkin's Vaccines

View all citing articles on Scopus

View full text

PaperTen-year neonatal hepatitis B vaccination program, the Netherlands, 1982–1992: protective efficacy and long-term immunogenicity

Abstract

Vaccine

Journal of Hepatology

Lancet

Vaccine

Lancet

Lancet

Lancet

Lancet

Passive-active immunisation of neonates of HBsAg positive carrier mothers: preliminary observations

British Medical Journal

Prevention of hepatitis B infection in newborns through mass screening and delayed vaccination of all infants of mothers with hepatitis B surface antigen

Pediatrics

Prevention of maternal-infant hepatitis B virus transmission by immunization: The role of serum hepatitis B virus DNA

Hepatology

Paper
Ten-year neonatal hepatitis B vaccination program, the Netherlands, 1982–1992: protective efficacy and long-term immunogenicity