HLA-A2 限制性细胞毒性 T 淋巴细胞对甲型流感病毒基质蛋白的识别。使用类似物确定基质肽在 HLA-A2 结合位点中的方向。
Recognition of influenza A matrix protein by HLA-A2-restricted cytotoxic T lymphocytes. Use of analogues to orientate the matrix peptide in the HLA-A2 binding site.
作者信息
Gotch F, McMichael A, Rothbard J
机构信息
Institute for Molecular Medicine, John Radcliffe Hospital, Oxford, United Kingdom.
出版信息
J Exp Med. 1988 Dec 1;168(6):2045-57. doi: 10.1084/jem.168.6.2045.
Abstract
CTL specific for the influenza A virus matrix peptide 57-68 and restricted by HLA-A2 were studied. Their ability to recognize a set of analogue peptides, each of which differed from the natural peptide by a single amino acid, was analyzed. This revealed a core of five amino acids, 61-65, where one or more changes completely abrogated recognition. The glycine at position 61 was the only residue where no substitution was tolerated. Analogue peptides that did not induce CTL-mediated lysis were tested as competitors with the natural peptide; those with substitutions at positions 60, 64, and 65 inhibited, identifying residues that interact with the TCR. Another approach was to test a set of four CTL clones on all of the analogues. Marked differences in recognition by individual CTL clones were observed for several substituted peptides. The data indicate that most of the analogues bind to HLA-A2 with possible differences in fine positioning of the peptide. An alpha helical orientation for the peptide is discussed.
摘要
对甲型流感病毒基质肽57 - 68具有特异性且受HLA - A2限制的细胞毒性T淋巴细胞(CTL)进行了研究。分析了它们识别一组类似肽的能力,每个类似肽与天然肽仅相差一个氨基酸。这揭示了一个由五个氨基酸(61 - 65)组成的核心,其中一个或多个变化会完全消除识别。61位的甘氨酸是唯一不能被取代的残基。未诱导CTL介导裂解的类似肽作为与天然肽竞争的物质进行测试;在60、64和65位有取代的那些肽具有抑制作用,确定了与T细胞受体(TCR)相互作用的残基。另一种方法是在所有类似物上测试一组四个CTL克隆。对于几个取代肽,观察到各个CTL克隆在识别上存在显著差异。数据表明,大多数类似物与HLA - A2结合,肽的精细定位可能存在差异。讨论了肽的α螺旋取向。
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