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一种用于估计全球乙型肝炎疾病负担和疫苗接种影响的数学模型。

A mathematical model to estimate global hepatitis B disease burden and vaccination impact.

作者信息

Goldstein Susan T, Zhou Fangjun, Hadler Stephen C, Bell Beth P, Mast Eric E, Margolis Harold S

机构信息

Division of Viral Hepatitis, Centers for Disease Control and Prevention, Atlanta, GA 30333, USA.

出版信息

Int J Epidemiol. 2005 Dec;34(6):1329-39. doi: 10.1093/ije/dyi206. Epub 2005 Oct 25.

Abstract

BACKGROUND

Limited data are available regarding global hepatitis B virus (HBV)-related morbidity and mortality and potential reduction in disease burden from hepatitis B vaccination.

METHODS

A model was developed to calculate the age-specific risk of acquiring HBV infection, acute hepatitis B (illness and death), and progression to chronic HBV infection. HBV-related deaths among chronically infected persons were determined from HBV-related cirrhosis and hepatocellular carcinoma (HCC) mortality curves, adjusted for background mortality. The effect of hepatitis B vaccination was calculated from vaccine efficacy and vaccination series coverage, with and without administration of the first dose of vaccine within 24 h of birth (i.e. birth dose) to prevent perinatal HBV infection.

RESULTS

For the year 2000, the model estimated 620,000 persons died worldwide from HBV-related causes: 580,000 (94%) from chronic infection-related cirrhosis and HCC and 40,000 (6%) from acute hepatitis B. In the surviving birth cohort for the year 2000, the model estimated that without vaccination, 64.8 million would become HBV-infected and 1.4 million would die from HBV-related disease. Infections acquired during the perinatal period, in early childhood (<5 years old), and > or = 5 years of age accounted for 21, 48, and 31% of deaths, respectively. Routine infant hepatitis B vaccination, with 90% coverage and the first dose administered at birth would prevent 84% of global HBV-related deaths.

CONCLUSION

Globally, most HBV-related deaths result from the chronic sequelae of infection acquired in the perinatal and early childhood periods. Inclusion of hepatitis B vaccine into national infant immunization programs could prevent >80% of HBV-related deaths.

摘要

背景

关于全球乙型肝炎病毒(HBV)相关的发病率、死亡率以及乙肝疫苗接种对疾病负担潜在降低作用的数据有限。

方法

建立了一个模型,用于计算特定年龄感染HBV的风险、急性乙型肝炎(发病和死亡)以及进展为慢性HBV感染的风险。慢性感染者中与HBV相关的死亡通过HBV相关肝硬化和肝细胞癌(HCC)死亡率曲线确定,并根据背景死亡率进行调整。根据疫苗效力和疫苗接种系列覆盖率计算乙肝疫苗接种的效果,接种分为出生后24小时内(即出生剂量)接种首剂疫苗和不接种首剂疫苗两种情况,以预防围产期HBV感染。

结果

对于2000年,该模型估计全球有62万人死于HBV相关原因:58万人(94%)死于慢性感染相关的肝硬化和HCC,4万人(6%)死于急性乙型肝炎。在2000年存活的出生队列中,该模型估计,若不接种疫苗,将有6480万人感染HBV,140万人死于HBV相关疾病。围产期、幼儿期(<5岁)和≥5岁期间获得的感染分别占死亡人数的21%、48%和31%。常规婴儿乙肝疫苗接种,覆盖率为90%且首剂在出生时接种,可预防全球84%的HBV相关死亡。

结论

在全球范围内,大多数HBV相关死亡是由围产期和幼儿期获得感染的慢性后遗症导致的。将乙肝疫苗纳入国家婴儿免疫规划可预防>80%的HBV相关死亡。

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