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抗轮状病毒免疫球蛋白A在通过上皮细胞转胞吞作用后可在体外中和病毒,并保护幼鼠免受腹泻之苦。

Antirotavirus immunoglobulin A neutralizes virus in vitro after transcytosis through epithelial cells and protects infant mice from diarrhea.

作者信息

Ruggeri F M, Johansen K, Basile G, Kraehenbuhl J P, Svensson L

机构信息

Laboratorio di Ultrastrutture, Istituto Superiore di Sanitá, Rome, Italy.

出版信息

J Virol. 1998 Apr;72(4):2708-14. doi: 10.1128/JVI.72.4.2708-2714.1998.

Abstract

Rotaviruses are the major cause of severe diarrhea in infants and young children worldwide. Due to their restricted site of replication, i.e., mature enterocytes, local intestinal antibodies have been proposed to play a major role in protective immunity. Whether secretory immunoglobulin A (IgA) antibodies alone can provide protection against rotavirus diarrhea has not been fully established. To address this question, a library of IgA monoclonal antibodies (MAbs) previously developed against different proteins of rhesus rotavirus was used. A murine hybridoma "backpack tumor" model was established to examine if a single MAb secreted onto mucosal surfaces via the normal epithelial transport pathway was capable of protecting mice against diarrhea upon oral challenge with rotavirus. Of several IgA and IgG MAbs directed against VP8 and VP6 of rotavirus, only IgA VP8 MAbs (four of four) were found to protect newborn mice from diarrhea. An IgG MAb recognizing the same epitope as one of the IgA MAbs tested failed to protect mice from diarrhea. We also investigated if antibodies could be transcytosed in a biologically active form from the basolateral domain to the apical domain through filter-grown Madin-Darby canine kidney (MDCK) cells expressing the polymeric immunoglobulin receptor. Only IgA antibodies with VP8 specificity (four of four) neutralized apically administered virus. The results support the hypothesis that secretory IgA antibodies play a major role in preventing rotavirus diarrhea. Furthermore, the results show that the in vivo and in vitro methods described are useful tools for exploring the mechanisms of viral mucosal immunity.

摘要

轮状病毒是全球婴幼儿严重腹泻的主要病因。由于其复制位点受限,即成熟肠上皮细胞,因此有人提出局部肠道抗体在保护性免疫中起主要作用。分泌型免疫球蛋白A(IgA)抗体单独是否能提供针对轮状病毒腹泻的保护作用尚未完全明确。为解决这个问题,使用了先前针对恒河猴轮状病毒不同蛋白开发的IgA单克隆抗体(MAb)文库。建立了小鼠杂交瘤“背包肿瘤”模型,以检查通过正常上皮转运途径分泌到粘膜表面的单一MAb在经轮状病毒口服攻击后是否能够保护小鼠免于腹泻。在几种针对轮状病毒VP8和VP6的IgA和IgG MAb中,仅发现IgA VP8 MAb(4/4)可保护新生小鼠免于腹泻。一种识别与所测试的一种IgA MAb相同表位的IgG MAb未能保护小鼠免于腹泻。我们还研究了抗体是否可以以生物活性形式通过表达多聚免疫球蛋白受体的滤过生长的Madin-Darby犬肾(MDCK)细胞从基底外侧结构域转胞吞至顶端结构域。仅具有VP8特异性的IgA抗体(4/4)中和了顶端施用的病毒。结果支持分泌型IgA抗体在预防轮状病毒腹泻中起主要作用的假设。此外,结果表明,所描述的体内和体外方法是探索病毒粘膜免疫机制的有用工具。

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