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甲型和乙型肝炎疫苗接种后的长期保护作用综述。

A review of the long-term protection after hepatitis A and B vaccination.

作者信息

Van Damme Pierre, Van Herck Koen

机构信息

Centre for the Evaluation of Vaccination, WHO Collaborating Centre for Prevention and Control of Viral Hepatitis, Department of Epidemiology and Social Medicine, University of Antwerp, Belgium.

出版信息

Travel Med Infect Dis. 2007 Mar;5(2):79-84. doi: 10.1016/j.tmaid.2006.04.004. Epub 2006 Jun 19.

Abstract

Vaccine-preventable viral hepatitis continues to be a cause of considerable morbidity and mortality: on worldwide basis, approximately 1.4 million cases of hepatitis A are reported every year. The true incidence, however, has been estimated to be 3-10 times higher. Regarding hepatitis B, more than a third of the world's population has been infected. The World Health Organization has estimated (2000) that there are 367 million chronic carriers of hepatitis B worldwide, and approximately 1 million deaths per year as a consequence of chronic complications and acute fulminant disease. Hepatitis B vaccines have been licensed since 1982, and hepatitis A vaccines since 1992. In 1996, a combined hepatitis A and B vaccine became available. An update on the long-term protection conferred by hepatitis A and hepatitis B vaccines as well as the combined hepatitis A and B vaccine is offered in this paper. Long-term efficacy and booster policy for hepatitis B vaccines have often been a topic of discussion. Based on current data and field experience there is, in general, no necessity for booster doses for fully vaccinated immunocompetent individuals. Long-term protection has been demonstrated by the rapid (5-7 days) development of anamnestic antibody responses among vaccinees who no longer have detectable anti-HBs. Anamnestic responses correlate with lymphoproliferative T-cell responses following challenge with hepatitis B vaccine. Furthermore, employing Spot-ELISA techniques, circulating B-cells were shown to be able to produce anti-HBs in vaccinees who lost their detectable antibodies. The accumulated data from a large number of studies indicate that despite antibody decline or loss, immune memory exhibits long-term persistence. There is somewhat less information available for hepatitis A vaccines, yet an increasing number of studies indicate that the findings for hepatitis B vaccines are also applicable to hepatitis A vaccines. The necessity to provide a booster dose was based on early projections of observed antibody levels. However, recent follow-up studies with up to 12 year observation, as well as studies employing mathematical models predict that following primary vaccination, antibodies will persist for at least 25 years. In addition, experimental studies confirm that vaccination against hepatitis A induces immunological memory. Therefore hepatitis A booster vaccination is presently considered as unnecessary in fully vaccinated individuals. The above findings are of importance in the context of administering combined hepatitis A and B vaccine for which similar long-term data have been observed. All available data on monovalent and combined hepatitis A and hepatitis B vaccines indicates that there is no support for a hepatitis A or hepatitis B booster when a complete primary vaccination course is offered to immunocompetent individuals.

摘要

疫苗可预防的病毒性肝炎仍然是导致相当高发病率和死亡率的原因

在全球范围内,每年报告约140万例甲型肝炎病例。然而,实际发病率估计要高出3至10倍。关于乙型肝炎,全球超过三分之一的人口已被感染。世界卫生组织(2000年)估计,全球有3.67亿慢性乙型肝炎携带者,每年约有100万人因慢性并发症和急性暴发性疾病死亡。乙型肝炎疫苗自1982年获得许可,甲型肝炎疫苗自1992年获得许可。1996年,一种甲型和乙型肝炎联合疫苗问世。本文提供了甲型和乙型肝炎疫苗以及甲型和乙型肝炎联合疫苗所提供的长期保护的最新情况。乙型肝炎疫苗的长期疗效和加强免疫策略一直是讨论的话题。根据目前的数据和现场经验,一般来说,对于完全接种疫苗的免疫功能正常的个体,没有必要进行加强剂量接种。在不再有可检测到的抗-HBs的疫苗接种者中,快速(5至7天)出现回忆性抗体反应证明了长期保护作用。回忆性反应与乙型肝炎疫苗激发后的淋巴细胞增殖性T细胞反应相关。此外,采用斑点酶联免疫吸附测定技术,在失去可检测抗体的疫苗接种者中,循环B细胞显示能够产生抗-HBs。大量研究积累的数据表明,尽管抗体水平下降或丧失,但免疫记忆仍长期存在。关于甲型肝炎疫苗的信息相对较少,但越来越多的研究表明,乙型肝炎疫苗的研究结果也适用于甲型肝炎疫苗。提供加强剂量的必要性是基于对观察到的抗体水平的早期预测。然而,最近长达12年观察期的随访研究以及采用数学模型的研究预测,初次接种疫苗后,抗体将持续至少25年。此外,实验研究证实,甲型肝炎疫苗接种可诱导免疫记忆。因此,目前认为对于完全接种疫苗的个体,没有必要进行甲型肝炎加强免疫接种。上述发现对于接种甲型和乙型肝炎联合疫苗具有重要意义,因为已观察到类似长期数据。关于单价和联合甲型和乙型肝炎疫苗的所有现有数据表明,当为免疫功能正常的个体提供完整的初次疫苗接种疗程时,没有支持进行甲型或乙型肝炎加强免疫接种的依据。

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