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一种由单克隆抗体定义的、所有HLA - B和HLA - C抗原共有的新型公共HLA I类表位的分子图谱。

Molecular mapping of a new public HLA class I epitope shared by all HLA-B and HLA-C antigens and defined by a monoclonal antibody.

作者信息

Trapani J A, Mizuno S, Kang S H, Yang S Y, Dupont B

机构信息

Laboratory of Human Immunogenetics, Memorial Sloan-Kettering Cancer Center, New York, NY 10021.

出版信息

Immunogenetics. 1989;29(1):25-32. doi: 10.1007/BF02341610.

Abstract

It has previously been shown that a mouse monoclonal antibody, designated 4E, reacts with an epitope common to all HLA-B and -C antigens and those of the HLA-Aw19 cross-reactive group, namely, HLA-A29, -A30, -A31, -A32, -Aw33, and -Aw74. In order to pinpoint the amino acid residues which comprise the public specificity recognized by 4E, and HLA-A29 cDNA clone was isolated and its predicted amino acid sequence compared with those of other cloned HLA class I genes. The isolated HLA-A29 cDNA corresponded to the rarer of the two A29 variant alleles, A29.1. Two amino acid residues of HLA-A29.1, gln-144 and arg-151, were found in all 24 HLA-B and HLA-C alleles examined but were present in only one of 15 HLA-A alleles for which sequence data are available. Importantly, this exceptional allele was HLA-A32, another member of the HLA-Aw19 cross-reactive group. Gln-144 and arg-151 should be capable of jointly contributing to the binding site for 4E, as they are situated in successive alpha-helical subregions and are predicted to be juxtaposed in the three-dimensional HLA molecule. Four other residues in the first or second external domains of HLA-A29.1 (thr-9, leu-62, gln-63, and his-102) were unique among the HLA-A alleles, but none of these was found in corresponding positions of HLA-B of -C alleles and thus failed to correlate with presence or absence of the 4E determinant. These observations are consistent with the notion that gln-144 and arg-151 define a determinant common to HLA-B, HLA-C, and the HLA-Aw19 cross-reactive group and the binding site of the monoclonal antibody 4E.

摘要

先前的研究表明,一种名为4E的小鼠单克隆抗体可与所有HLA - B和 - C抗原以及HLA - Aw19交叉反应组(即HLA - A29、 - A30、 - A31、 - A32、 - Aw33和 - Aw74)的抗原所共有的一个表位发生反应。为了确定构成4E所识别的公共特异性的氨基酸残基,分离出了一个HLA - A29 cDNA克隆,并将其预测的氨基酸序列与其他克隆的HLA I类基因的序列进行比较。分离出的HLA - A29 cDNA对应于两个A29变异等位基因中较罕见的那个,即A29.1。在所有检测的24个HLA - B和HLA - C等位基因中都发现了HLA - A29.1的两个氨基酸残基,即谷氨酰胺 - 144和精氨酸 - 151,但在15个有序列数据的HLA - A等位基因中,只有一个存在这两个残基。重要的是,这个特殊的等位基因是HLA - A32,它是HLA - Aw19交叉反应组的另一个成员。谷氨酰胺 - 144和精氨酸 - 151应该能够共同构成4E的结合位点,因为它们位于连续的α - 螺旋亚区域,并且预计在三维HLA分子中是并列的。HLA - A29.1的第一或第二外部结构域中的其他四个残基(苏氨酸 - 9、亮氨酸 - 62、谷氨酰胺 - 63和组氨酸 - 102)在HLA - A等位基因中是独特的,但在HLA - B或 - C等位基因的相应位置均未发现,因此与4E决定簇的存在与否无关。这些观察结果与以下观点一致,即谷氨酰胺 - 144和精氨酸 - 151定义了一个HLA - B、HLA - C和HLA - Aw19交叉反应组所共有的决定簇以及单克隆抗体4E的结合位点。

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