Publication: Immunogenicity and protective efficacy of low dose recombinant DNA hepatitis B vaccine in normal and high-risk neonates
Issued Date
1991-12-01
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ISSN
0125877X
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2-s2.0-0026344412
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Mahidol University
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SCOPUS
Bibliographic Citation
Asian Pacific Journal of Allergy and Immunology. Vol.9, No.2 (1991), 89-93
Suggested Citation
A. Assateerawatt, V. S. Tanphaichitr, V. Suvatte, L. In-ngarm Immunogenicity and protective efficacy of low dose recombinant DNA hepatitis B vaccine in normal and high-risk neonates. Asian Pacific Journal of Allergy and Immunology. Vol.9, No.2 (1991), 89-93. Retrieved from: https://repository.li.mahidol.ac.th/handle/20.500.14594/22040
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Title
Immunogenicity and protective efficacy of low dose recombinant DNA hepatitis B vaccine in normal and high-risk neonates
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Abstract
A low dose of recombinant DNA hepatitis B vaccine (HB-VAX II®, MSD) was tested for efficacy in the prevention of perinatal hepatitis B virus (HBV) transmission in normal and high-risk neonates born from HBsAg carrier mothers. A dose of 2.5 μg recombinant vaccine was injected intramuscularly at 0, 1, 2 and 12 months of age to 30 newborns from HBsAg negative mother (group I), 30 from HBeAg negative/HBsAg carrier mother (group II) and 30 from HBeAg positive/HBsAg carrier mother (group III). The incidence of persistent HBsAg carrier infants at 13 months of age was 0, 0, and 30.4 percent in groups I, II and III, respectively. The protective efficacy in high risk infants in group III was 65.7 percent. The seroconversion at month 4, after the third dose of vaccination was 96.3, 95.7 and 100 percent in group I, group II and group III, respectively. After a booster dose of vaccination at 12 months of age, the seroconversion rose to 100 percent at month 13 in all three groups. The geometric mean titer (GMT) of anti-HBs antibody at 13 months of age were 2,092, 1,657 and 1,938 mIU/ml in group I, group II and group III, respectively. It is concluded that the low dose (2.5 μg) recombinant hepatitis B vaccine using alone is effective in prevention of perinatal HBV transmission in low risk infants (groups I and II), but it is less effective in high risk infants (group III). The low dose hepatitis B vaccine regimen should be combined with HBIG given at birth for the full protection of perinatal HBV transmission in the high risk neonates born from the HBeAg positive/HBsAg carrier mothers which comprised approximately 3 percent of all newborns in the endemic area. This approach would certainly reduce the cost of hepatitis B immunization and it could be applied economically for the national program of HBV transmission control in neonates.