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儿童自然初次感染和再次感染轮状病毒后针对轮状病毒蛋白的同型和异型血清中和抗体反应。

Homotypic and heterotypic serum neutralizing antibody response to rotavirus proteins following natural primary infection and reinfection in children.

作者信息

Gorrell R J, Bishop R F

机构信息

Department of Gastroenterology and Clinical Nutrition, Royal Children's Hospital, Parkville, Victoria, Australia.

出版信息

J Med Virol. 1999 Feb;57(2):204-11.

PMID:9892409
Abstract

Worldwide trials of rotavirus vaccines are currently in progress, but the basis of cross-reactive immunity between rotavirus serotypes is yet to be elucidated. The involvement of the outer capsid proteins, VP7 and VP4, in the production of cross-reactive neutralizing antibody (N-Ab) is unclear, and may be important for the success of animal rotavirus-based candidate vaccines that lack a VP4 of human rotavirus origin. In this study, VP7- and VP4-specific N-Ab was assayed in sera from children experiencing primary (27 children) and/or secondary (14 children) rotavirus infections using human-animal reassortant strains. These reassortants contained genes encoding the major G- and P-types found in human infection, including G1, 2, 3, and 4; or P1A[8], 1B[4], and 2[6]. After primary infection, the N-Ab response to VP7 was generally serotype-specific, whereas the response to VP4 was heterotypic. After reinfection (with the same or different serotypes) there was a significant increase (P=0.0313) in the number of VP7 serotypes seroconverted against with no broadening of cross-reactivity to VP4. Increases in homotypic N-Ab titer, following both primary and secondary infection, were greater against VP7 than VP4, with the seroconversion against VP7 being significantly greater upon reinfection than following primary infection (P=0.0280). In summary, heterotypic N-Ab produced following primary infection appears to be primarily against VP4. However, upon reinfection, VP7 becomes increasingly immunodominant both in terms of cross-reactive N-Ab production and increases in N-Ab titer.

摘要

目前全球范围内正在进行轮状病毒疫苗试验,但轮状病毒各血清型之间交叉反应性免疫的基础仍有待阐明。外壳蛋白VP7和VP4在交叉反应性中和抗体(N-Ab)产生中的作用尚不清楚,这对于缺乏人源轮状病毒VP4的动物源轮状病毒候选疫苗的成功可能很重要。在本研究中,使用人-动物重配株检测了初次感染(27名儿童)和/或二次感染(14名儿童)轮状病毒的儿童血清中VP7和VP4特异性N-Ab。这些重配株包含编码人类感染中发现的主要G型和P型的基因,包括G1、2、3和4;或P1A[8]、1B[4]和2[6]。初次感染后,对VP7的N-Ab反应通常具有血清型特异性,而对VP4的反应是异型的。再次感染(相同或不同血清型)后,VP7血清型血清转化的数量显著增加(P=0.0313),但对VP4的交叉反应性没有拓宽。初次和二次感染后,同型N-Ab滴度的增加对VP7的反应比对VP4的反应更大,再次感染时针对VP7的血清转化比初次感染时显著更大(P=0.0280)。总之,初次感染后产生的异型N-Ab似乎主要针对VP4。然而,再次感染时,无论是在交叉反应性N-Ab产生还是N-Ab滴度增加方面,VP7都变得越来越具有免疫优势。

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