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由针对拉沙病毒包膜糖蛋白表位的CD4 + T细胞克隆介导的对淋巴细胞性脉络丛脑膜炎病毒的交叉保护作用。

Cross-protection against lymphocytic choriomeningitis virus mediated by a CD4+ T-cell clone specific for an envelope glycoprotein epitope of Lassa virus.

作者信息

La Posta V J, Auperin D D, Kamin-Lewis R, Cole G A

机构信息

Department of Microbiology and Immunology, University of Maryland, Baltimore 21201.

出版信息

J Virol. 1993 Jun;67(6):3497-506. doi: 10.1128/JVI.67.6.3497-3506.1993.

Abstract

Recombinant vaccinia virus expressing the Lassa virus (LV) envelope glycoprotein precursor, V-LSGPC, was used to study the basis of LV-induced cross-protective immunity against the closely related arenavirus lymphocytic choriomeningitis virus (LCMV). C3H/HeJ mice primed with V-LSGPC developed neither circulating antibodies nor CD8+ cytotoxic T cells specific for LCMV, yet they resisted a normally lethal LCMV challenge. Spleen cells from such mice gave a proliferative response to LCMV in vitro that was inhibitable by anti-CD4 antibody. Synthetic peptides corresponding to predicted T-cell sites common to the envelope glycoprotein precursor (GP-C) of LV and that of LCMV were used to map the specificity of the proliferative response to an epitope located between amino acids 403 and 417 of LV GP-C. Several CD4+ T-cell clones specific for the 403-417 peptide were isolated and found to produce gamma interferon in response to both the peptide and LCMV. One of these clones, C9, was selected for further study. C9 lysed I-AK-bearing target cells, and when adoptively transferred to C3H/HeJ mice, it was capable of mediating both a peptide-specific delayed hypersensitivity reaction and resistance to lethal LCMV challenge. These collective findings demonstrate, for the first time, that CD4+ T cells can play a major role in arenavirus-specific cross-protective immunity.

摘要

表达拉沙病毒(LV)包膜糖蛋白前体的重组痘苗病毒V-LSGPC,被用于研究LV诱导的针对密切相关的沙粒病毒淋巴细胞性脉络丛脑膜炎病毒(LCMV)的交叉保护性免疫的基础。用V-LSGPC免疫的C3H/HeJ小鼠既不产生针对LCMV的循环抗体,也不产生特异性CD8 + 细胞毒性T细胞,但它们能够抵抗通常致死剂量的LCMV攻击。来自此类小鼠的脾细胞在体外对LCMV产生增殖反应,该反应可被抗CD4抗体抑制。与LV和LCMV包膜糖蛋白前体(GP-C)共有的预测T细胞位点对应的合成肽,被用于将增殖反应的特异性定位到LV GP-C氨基酸403和417之间的一个表位。分离出了几个对403-417肽特异的CD4 + T细胞克隆,发现它们对该肽和LCMV均产生γ干扰素反应。其中一个克隆C9被选作进一步研究。C9可裂解表达I-AK的靶细胞,当将其过继转移到C3H/HeJ小鼠时,它能够介导肽特异性迟发型超敏反应和对致死性LCMV攻击的抵抗力。这些总体发现首次证明,CD4 + T细胞在沙粒病毒特异性交叉保护性免疫中可发挥主要作用。

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