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一种为在发展中国家使用而设计的六价人轮状病毒-牛轮状病毒(英国)重组疫苗,其接种程序有可能消除肠套叠风险。

A hexavalent human rotavirus-bovine rotavirus (UK) reassortant vaccine designed for use in developing countries and delivered in a schedule with the potential to eliminate the risk of intussusception.

作者信息

Kapikian Albert Z, Simonsen Lone, Vesikari Timo, Hoshino Yasutaka, Morens David M, Chanock Robert M, La Montagne John R, Murphy Brian R

机构信息

National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

J Infect Dis. 2005 Sep 1;192 Suppl 1:S22-9. doi: 10.1086/431510.

Abstract

There is an urgent need for a rotavirus vaccine, because up to 592,000 infants and young children <5 years old die each year from rotavirus diarrhea, predominantly in the developing countries. We have developed a tetravalent human-bovine rotavirus (UK) reassortant vaccine with VP7 (G) specificity for serotypes 1, 2, 3, and 4, which has been shown to be safe, immunogenic, and effective in preventing severe rotavirus diarrhea. However, because of the emergence of VP7 (G) serotype 9 as an epidemiologically important serotype and the importance of VP7 (G) serotype 8 in focal areas, we are planning to add human-bovine (UK) reassortants with G8 and G9 specificity to the tetravalent vaccine, thereby formulating a "designed" hexavalent vaccine for universal use. In addition, we propose that the vaccine be administered orally in a 2-dose schedule, with the first dose given at 0-4 weeks of age and the second dose given at 4-8 weeks of age, when infants are relatively refractory to developing intussusception, thereby avoiding the age period when naturally occurring intussusception is most prevalent (i.e., ages 3-4 months through age 9 months). In this way, there may be the potential to eliminate or at least significantly decrease the risk of intussusception associated with rotavirus vaccination.

摘要

迫切需要一种轮状病毒疫苗,因为每年有多达59.2万名5岁以下婴幼儿死于轮状病毒腹泻,主要发生在发展中国家。我们研发了一种四价人-牛轮状病毒(英国)重配疫苗,对1、2、3和4型具有VP7(G)特异性,已证明该疫苗在预防严重轮状病毒腹泻方面安全、具有免疫原性且有效。然而,由于VP7(G)9型已成为具有流行病学重要性的血清型,且VP7(G)8型在局部地区也很重要,我们计划在四价疫苗中添加具有G8和G9特异性的人-牛(英国)重配体,从而制备一种通用的“设计”六价疫苗。此外,我们建议该疫苗采用2剂口服接种程序,第一剂在0至4周龄时接种,第二剂在4至8周龄时接种,此时婴儿发生肠套叠的可能性相对较低,从而避开自然发生肠套叠最普遍的年龄段(即3至4个月龄至9个月龄)。通过这种方式,有可能消除或至少显著降低与轮状病毒疫苗接种相关的肠套叠风险。

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