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HIV-1 整合酶特异性 HLA-B∗4002 限制性 T 细胞对 HIV-1 感染细胞的有效识别。

Effective recognition of HIV-1-infected cells by HIV-1 integrase-specific HLA-B∗4002-restricted T cells.

机构信息

Center for AIDS Research, Kumamoto University, 2-2-1 Honjo, Kumamoto 860-0811, Japan.

出版信息

Microbes Infect. 2011 Feb;13(2):160-6. doi: 10.1016/j.micinf.2010.10.006. Epub 2010 Nov 4.

Abstract

HLA-B∗4002 is one of the common HLA-B alleles in the world. All 7 reported HLA-B∗4002-restricted HIV epitopes are derived from Gag, Nef, and Vpr. In the present study we sought to identify novel HLA-B∗4002-restricted HIV epitopes by using overlapping 11-mer peptides of HIV-1 Nef, Gag, and Pol, and found that 6 of these 11-mer Pol peptides included HLA-B∗4002-restricted epitopes. Analysis using truncated peptides of these 6 peptides defined 4 optimal Pol (integrase) epitopes. All epitopes previously reported had Glu at position 2 (P2), suggesting that Glu at P2 is the anchor residue for HLA-B∗4002; whereas only 2 of the integrase epitopes that we here identified had Glu at P2. CTL clones specific for the 2 epitopes effectively recognized HIV-1-infected cells whereas those for other 2 epitopes only weakly recognized them. The antigen sensitivity of the former clones for the epitope peptide was much higher than that of the latter clones, suggesting 2 possibilities: 1) the former T cells have high-affinity TCRs and/or 2) the epitope peptides recognized by the former T cells are highly presented by HLA-B∗4002 in HIV-1-infected cells. These integrase-specific T cells with high antigen sensitivity may contribute to the suppression of HIV-1 replication in HIV-1-infected HLA-B∗4002+ individuals.

摘要

HLA-B∗4002 是世界上常见的 HLA-B 等位基因之一。所有已报道的 7 个受 HLA-B∗4002 限制的 HIV 表位均来自 Gag、Nef 和 Vpr。在本研究中,我们试图通过使用重叠的 HIV-1 Nef、Gag 和 Pol 的 11 聚体肽来鉴定新的受 HLA-B∗4002 限制的 HIV 表位,发现这些 11 聚体 Pol 肽中有 6 个包含受 HLA-B∗4002 限制的表位。对这些 6 个肽的截断肽进行分析,确定了 4 个最佳的 Pol(整合酶)表位。以前报道的所有表位在位置 2(P2)都有谷氨酸,这表明 P2 的谷氨酸是 HLA-B∗4002 的锚定残基;而我们在这里鉴定的整合酶表位中只有 2 个有 P2 的谷氨酸。针对这 2 个表位的 CTL 克隆能有效识别感染 HIV-1 的细胞,而针对其他 2 个表位的 CTL 克隆只能弱识别它们。前一组克隆对表位肽的抗原敏感性比后一组克隆高得多,这表明有 2 种可能性:1)前一组 T 细胞具有高亲和力的 TCR,和/或 2)前一组 T 细胞识别的表位肽在感染 HIV-1 的细胞中由 HLA-B∗4002 高度呈递。这些具有高抗原敏感性的整合酶特异性 T 细胞可能有助于抑制 HIV-1 复制。

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