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Identification of overlapping HLA class I-restricted cytotoxic T cell epitopes in a conserved region of the human immunodeficiency virus type 1 envelope glycoprotein: definition of minimum epitopes and analysis of the effects of sequence variation

机译:鉴定人类免疫缺陷病毒1型包膜糖蛋白保守区中重叠的HLA I类限制性细胞毒性T细胞表位:最小表位的定义和序列变异的影响分析

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摘要

Although the immunologic basis of protective immunity in human immunodeficiency virus type 1 (HIV-1) infection has not yet been defined, virus-specific cytotoxic T lymphocytes (CTL) are likely to be an important host defense and may be a critical feature of an effective vaccine. These observations, along with the inclusion of the HIV-1 envelope in the majority of vaccine candidates presently in clinical trials, underscore the importance of the precise characterization of the cellular immune responses to this protein. Although humoral immune responses to the envelope protein have been extensively characterized, relatively little information is available regarding the envelope epitopes recognized by virus-specific CTL and the effects of sequence variation within these epitopes. Here we report the identification of two overlapping CTL epitopes in a highly conserved region of the HIV-1 transmembrane envelope protein, gp41, using CTL clones derived from two seropositive subjects. An eight-amino acid peptide was defined as the minimum epitope recognized by HLA-B8-restricted CTL derived from one subject, and in a second subject, an overlapping nine-amino acid peptide was identified as the minimal epitope for HLA-B14-restricted CTL clones. Selected single amino acid substitutions representing those found in naturally occurring HIV-1 isolates resulted in partial to complete loss of recognition of these epitopes. These data indicate the presence of a highly conserved region in the HIV-1 envelope glycoprotein that is immunogenic for CTL responses. In addition, they suggest that natural sequence variation may lead to escape from immune detection by HIV-1-specific CTL. Since the region containing these epitopes has been previously shown to contain an immunodominant B cell epitope and also overlaps with a major histocompatibility complex class II T cell epitope recognized by CD4+ CTL from HIV-1 rgp160 vaccine recipients, it may be particularly important for HIV-1 vaccine development. Finally, the identification of minimal CTL epitopes presented by class I HLA molecules should facilitate the definition of allele-specific motifs.
机译:尽管尚未定义1型人类免疫缺陷病毒(HIV-1)感染中保护性免疫的免疫学基础,但病毒特异性细胞毒性T淋巴细胞(CTL)可能是重要的宿主防御系统,可能是肝癌的重要特征。有效疫苗。这些观察结果以及目前临床试验中大多数候选疫苗中都包含HIV-1包膜,突显了精确表征对该蛋白的细胞免疫反应的重要性。尽管对包膜蛋白的体液免疫反应已得到广泛表征,但有关病毒特异性CTL识别的包膜表位以及这些表位中序列变异的影响的信息相对较少。在这里,我们报告使用两个血清阳性患者的CTL克隆,鉴定HIV-1跨膜包膜蛋白gp41的高度保守区域中两个重叠的CTL表位。八氨基酸肽定义为由一名受试者衍生的HLA-B8限制性CTL识别的最小表位,在第二名受试者中,重叠的九氨基酸肽被鉴定为HLA-B14限制性的最小表位CTL克隆。代表在天然存在的HIV-1分离物中发现的代表的选定单个氨基酸取代,导致部分或完全丧失了对这些表位的识别。这些数据表明HIV-1包膜糖蛋白中存在高度保守的区域,该区域对CTL反应具有免疫原性。此外,他们认为自然序列变异可能导致无法通过HIV-1特异性CTL进行免疫检测。由于先前已证明包含这些表位的区域含有免疫优势的B细胞表位,并且还与CD4 + CTL识别的来自HIV-1 rgp160疫苗接受者的主要组织相容性复合物II类T细胞表位重叠,因此对于HIV- 1疫苗开发。最后,由I类HLA分子呈现的最小CTL表位的鉴定应有助于定义等位基因特异性基序。

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  • 年度 1992
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