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在用嵌合VP6蛋白和佐剂LT(R192G)进行鼻内免疫后,CD4 T细胞是保护小鼠免受轮状病毒脱落所需的唯一淋巴细胞。

CD4 T cells are the only lymphocytes needed to protect mice against rotavirus shedding after intranasal immunization with a chimeric VP6 protein and the adjuvant LT(R192G).

作者信息

McNeal Monica M, VanCott John L, Choi Anthony H C, Basu Matili, Flint Jason A, Stone Susan C, Clements John D, Ward Richard L

机构信息

Division of Infectious Diseases, Children's Hospital Medical Center, Cincinnati, Ohio 45229, USA.

出版信息

J Virol. 2002 Jan;76(2):560-8. doi: 10.1128/jvi.76.2.560-568.2002.

Abstract

Intranasal immunization of mice with a chimeric VP6 protein and the mucosal adjuvant Escherichia coli heat labile toxin LT(R192G) induces nearly complete protection against murine rotavirus (strain EDIM [epizootic diarrhea of infant mice virus]) shedding for at least 1 year. The aim of this study was to identify the protective lymphocytes elicited by this new vaccine candidate. Immunization of mouse strains lacking one or more lymphocyte populations revealed that protection was dependent on alphabeta T cells but mice lacking gammadelta T cells and B cells remained fully protected. Furthermore, depletion of CD8 T cells in immunized B-cell-deficient mice before challenge resulted in no loss of protection, while depletion of CD4 T cells caused complete loss of protection. Therefore, alphabeta CD4 T cells appeared to be the only lymphocytes required for protection. As confirmation, purified splenic T cells from immunized mice were intraperitoneally injected into Rag-2 mice chronically infected with EDIM. Transfer of 2 x 10(6) CD8 T cells had no effect on shedding, while transfer of 2 x 10(5) CD4 T cells fully resolved shedding in 7 days. Interestingly, transfer of naive splenic CD4 T cells also resolved shedding but more time and cells were required. Together, these results establish CD4 T cells as effectors of protection against rotavirus after intranasal immunization of mice with VP6 and LT(R192G).

摘要

用嵌合VP6蛋白和黏膜佐剂大肠杆菌不耐热毒素LT(R192G)对小鼠进行鼻内免疫,可诱导产生近乎完全的保护作用,使小鼠轮状病毒(EDIM株[幼鼠流行性腹泻病毒])的排毒至少在1年内受到抑制。本研究的目的是鉴定这种新型候选疫苗所引发的保护性淋巴细胞。对缺乏一种或多种淋巴细胞群体的小鼠品系进行免疫,结果显示保护作用依赖于αβ T细胞,但缺乏γδ T细胞和B细胞的小鼠仍能得到完全保护。此外,在攻击前对免疫的B细胞缺陷小鼠中的CD8 T细胞进行清除,并未导致保护作用丧失,而清除CD4 T细胞则导致保护作用完全丧失。因此,αβ CD4 T细胞似乎是保护作用所需的唯一淋巴细胞。作为证实,将免疫小鼠的纯化脾T细胞腹腔注射到长期感染EDIM的Rag-2小鼠体内。转移2×10⁶个CD8 T细胞对病毒排毒没有影响,而转移2×10⁵个CD4 T细胞在7天内完全消除了病毒排毒。有趣的是,转移未活化的脾CD4 T细胞也能消除病毒排毒,但需要更多时间和细胞。总之,这些结果确立了CD4 T细胞是小鼠用VP6和LT(R192G)进行鼻内免疫后抗轮状病毒保护作用的效应细胞。

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