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针对HIV-1 gp120免疫显性C5区域的人抗体与活化细胞上的HLA I类分子发生交叉反应。

Human antibodies to immunodominant C5 region of HIV-1 gp120 cross-react with HLA class I on activated cells.

作者信息

de Santis C, Lopalco L, Robbioni P, Longhi R, Rappocciolo G, Siccardi A G, Beretta A

机构信息

DIBIT, Dipartimento di Ricerca Biologica e Tecnologica, Ospedale San Raffaele, Milan, Italy.

出版信息

AIDS Res Hum Retroviruses. 1994 Feb;10(2):157-62. doi: 10.1089/aid.1994.10.157.

Abstract

Cross-reactive antibodies to HLA class I and HIV-1 gp120 were detected in the sera of HIV-1-positive individuals, and were found to share the same epitope specificity as a gp120-HLA class I cross-reactive monoclonal antibody (M38). The amino acid residues of HLA recognized by both M38 and the patient antibodies occur as a clustered pair in the HLA-C alpha 1 domain. These sequences (KYKR and RKLR) are shared by almost all HLA-C alleles and are available to antibody binding only on beta 2-microglobulin-dissociated HLA heavy chains expressed on activated cells. Similar to M38, the antibody-binding sites on HIV-1 gp120 were mapped to two noncontiguous stretches of amino acids (KYK and KAKR), which flank a hydrophobic area of the immunodominant C5 region involved in gp41 binding. Serum antibodies immunoaffinity purified on synthetic HLA and gp120 peptides representing the M38-reactive regions were shown to bind to both HLA and gp120 in Western blot, as well as to membrane-bound HLA heavy chains, and to exhibit selective complement-mediated lysis of activated T cells. No serum antibodies could be detected that bind to the gp120 C5 region (peptide IEPLGVAPT) flanked by the two HLA-like sequences.

摘要

在HIV-1阳性个体的血清中检测到了针对HLA I类分子和HIV-1 gp120的交叉反应性抗体,并且发现这些抗体与一种gp120-HLA I类分子交叉反应性单克隆抗体(M38)具有相同的表位特异性。M38和患者抗体所识别的HLA氨基酸残基在HLA-C α1结构域中呈簇状配对出现。这些序列(KYKR和RKLR)几乎为所有HLA-C等位基因所共有,并且仅在活化细胞上表达的β2-微球蛋白解离的HLA重链上可用于抗体结合。与M38相似,HIV-1 gp120上的抗体结合位点被定位到两个不连续的氨基酸片段(KYK和KAKR),它们位于参与gp41结合的免疫显性C5区域的一个疏水区域两侧。在代表M38反应区域的合成HLA和gp120肽上进行免疫亲和纯化的血清抗体,在蛋白质印迹中显示既能结合HLA也能结合gp120,还能结合膜结合的HLA重链,并表现出对活化T细胞的选择性补体介导的裂解作用。未检测到能结合位于两个类HLA序列两侧的gp120 C5区域(肽IEPLGVAPT)的血清抗体。

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