Observational Study of Vaccine Efficacy 24 Years after the Start of Hepatitis B Vaccination in Two Gambian Villages: No Need for a Booster Dose

被引:95
作者
Mendy, Maimuna [1 ]
Peterson, Ingrid [1 ]
Hossin, Safayet [1 ]
Peto, Tom [1 ]
Jobarteh, Momodou L. [1 ]
Jeng-Barry, Adam [1 ]
Sidibeh, Mamadi [1 ]
Jatta, Abdoulie [1 ]
Moore, Sophie E. [2 ]
Hall, Andrew J. [3 ]
Whittle, Hilton [1 ,3 ]
机构
[1] MRC Labs, Banjul, Gambia
[2] MRC Keneba, MRC Unit, Banjul, Gambia
[3] London Sch Hyg & Trop Med, London WC1, England
关键词
VIRUS-INFECTION; HEPATOCELLULAR-CARCINOMA; SURFACE-ANTIGEN; CHILDREN BORN; HBV; ANTIBODY; TRIAL; IMMUNIZATION; PREVALENCE; PROTECTION;
D O I
10.1371/journal.pone.0058029
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Objectives: To determine the duration of protection from hepatitis B vaccine given in infancy and early childhood and asses risk factors for HBV infection and chronic infection. Methods: In 1984 infant HBV vaccination was started in two Gambian villages. Cross sectional serological surveys have been undertaken every 4 years to determine vaccine efficacy. In the current survey 84.6% of 1508 eligible participants aged 128 years were tested. A spouse study was conducted in females (aged 14 years and above) and their male partners. Results: Vaccine efficacy against chronic infection with hepatitis B virus was 95.1% (95% confidence interval 91.5% to 97.1%), which did not vary significantly between age groups or village. Efficacy against infection was 85.4% (82.7% to 87.7%), falling significantly with age. Concentrations of hepatitis B antibody fell exponentially with age varying according to peak response: 20 years after vaccination only 17.8% (95% Cl 10.1-25.6) of persons with a low peak response (10-99 mIU/ml) had detectable HBs antibody compared to 27% (21.9% to 32.2%) of those with a high peak response (>999 mIU/ml). Time since vaccination and a low peak response were the strongest risk factors for HBV infections; males were more susceptible, marriage was not a significant risk for females. Hepatitis B DNA was not detected after infection, which tested soley core antibody positive. An undetectable peak antibody response of <10 mIU/ml and a mother who was hepatitis B e antigen positive were powerful risk factors for chronic infection. Conclusions: Adolescents and young adults vaccinated in infancy are at increased risk of hepatitis B infection, but not chronic infection. Married women were not at increased risk. There is no compelling evidence for the use of a booster dose of HBV vaccine in The Gambia.
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