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Journal ArticleDOI

Nine-year follow-up study of a plasma-derived hepatitis B vaccine in a rural African setting.

TLDR
Data support the long‐term immunogenicity and protective efficacy of a two‐ or three‐dose regimen of the hepatitis B vaccine in a rural African setting.
Abstract
One hundred and one of 255 recipients of a plasma-derived hepatitis B vaccine were evaluated in 1990, 9 years after the first vaccine dose in a study in Zambia to evaluate the efficacy of one, two, or three doses. In 1983, 2 years after the first vaccine dose, antibody to the hepatitis B surface antigen (anti-HBs) had been detectable in 90 of these 101 participants (89%). In 1990, anti-HBs was still detectable in 72 of 101 (71%), and was present at a protective level ( ≥ 10 mlU ml) in 68 of 101 (67%). Although the original vaccine study elicited a protective level of antibody in a greater percentage of children and adolescents than in adults, there were no significant differences among the three groups at 9 years. (In 1990, anti-HBs was still detectable in 52 of 70 [74%] who had had no serologic markers of the hepatitis B virus in 1981, and a protective level was detected in 47 of 70 [67%].) A protective level of anti-HBs was detected in 1990 in 26 of 36 (72%) recipients of three doses and in 23 of 31 (74%) recipients of two doses; the slightly lower prevalence among recipients of one dose (19 of 34 [56%]) was not statistically significant. However, between the years 1983–1990, hepatitis B virus infections had occurred in one of 36 (3%) of those who had been vaccinated with three doses, one of 31 (3%) vaccinated with two doses, and eight of 34 (24%) of those vaccinated with one dose (P < .02 for either two or three doses compared with one dose). These data support the long-term immunogenicity and protective efficacy of a two- or three-dose regimen of the hepatitis B vaccine in a rural African setting. © 1993 Wiley-Liss, Inc.

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Antibody levels and protection after hepatitis B vaccination: results of a 15-year follow-up

TL;DR: Data is reported on the persistence of antibodies to hepatitis B surface antigen (anti-HBs), incidence of HBV infection, and the genetic characteristics of the HBV isolates in persons with breakthrough infections 15 years after initial vaccination of this cohort.
Journal ArticleDOI

Protection Provided by Hepatitis B Vaccine in a Yupik Eskimo Population—Results of a 10-Year Study

TL;DR: It is suggested that immunization with hepatitis B vaccine continues to provide high levels of protection from clinical disease for at least 10 years.
Journal ArticleDOI

Incidence of type 2 diabetes in the randomized multiple risk factor intervention trial.

TL;DR: The incidence of diabetes is compared in the intervention and control groups of the MRFIT, an unexpected subgroup finding related to baseline cigarette smoking status is reported, and reasons for the different results among smokers and nonsmokers are explored.
Journal ArticleDOI

Progression of liver fibrosis in women infected with hepatitis C: long-term benefit of estrogen exposure.

TL;DR: Di Martino et al. as discussed by the authors examined estrogen-related effects on hepatitis C fibrosis in a cross-sectional cohort study and found that progression of hepatitis C was correlated with prior pregnancies, menopausal status, past use of oral contraceptives, and hormone replacement therapy.
References
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Journal ArticleDOI

Duration of immunogenicity and efficacy of hepatitis B vaccine in a Yupik Eskimo population.

TL;DR: In 1981, a hepatitis B virus vaccine demonstration project was conducted in 1630 Yupik Eskimos in southwest Alaska, and in the 5 years following the demonstration project, the annual incidence of hepatitis Birus infection decreased from 50 cases per 1000 population before the vaccine trial to 0.45 per 1000.
Journal ArticleDOI

The immune response of healthy adults to a reduced dose of hepatitis B vaccine.

TL;DR: Three hundred thirty‐six medical personnel from hemodialysis centers treated with three doses, 20 μg each, of the Merck hepatitis B vaccine (at 0, 1, and 6 months) converted to anti‐HBs positivity within 1 month after the first injection, and the later rate remained unchanged during the 18‐month follow‐up period.
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