| Literature DB >> 7715343 |
H C Whittle1, N Maine, J Pilkington, M Mendy, M Fortuin, J Bunn, L Allison, C Howard, A Hall.
Abstract
In 1984, all non-immune children under the age of 5 years in the Gambian villages of Keneba and Manduar were vaccinated against hepatitis B virus (HBV). All children born in these villages since 1984 have been vaccinated in infancy. Despite a rapid fall in antibody concentrations, vaccine efficacy against HBV infection and chronic carriage of HBsAg has increased with time. Overall, vaccine efficacies in 1993 against HBV infection and chronic HBsAg carriage were 94.7% (95% Cl 93.0-96.0) and 95.3% (91.0-97.5), respectively. Breakthrough infections in vaccinated children largely originate from chronic HBsAg carriers. Thus, we tested 261 chronic carriers for HBV DNA and e antigen. The prevalence of these markers of infectivity, and the amount of HBV DNA, decreased greatly with age. Detailed studies of breakthrough infections over two 4-year periods revealed that in the second period there were fewer than half the expected numbers of infections. Our findings suggest that in Keneba and Manduar long-term vaccination is progressively decreasing HBV transmission by chronic carriers, since their infectivity diminishes with time.Entities:
Keywords: Africa; Africa South Of The Sahara; Antibodies; Biology; Delivery Of Health Care; Developing Countries; Diseases; English Speaking Africa; Examinations And Diagnoses; Follow-up Studies; Gambia; Health; Health Services; Hepatitis--prevention and control; Immunity; Immunization; Immunologic Factors; Laboratory Examinations And Diagnoses; Physiology; Primary Health Care; Program Effectiveness; Program Evaluation; Programs; Research Report; Studies; Vaccination; Viral Diseases; Western Africa
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Year: 1995 PMID: 7715343 DOI: 10.1016/s0140-6736(95)90822-6
Source DB: PubMed Journal: Lancet ISSN: 0140-6736 Impact factor: 79.321