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一种新的HLA - B27等位基因将B27同种特异性定位到α1结构域中第70位左右的区域。

A novel HLA-B27 allele maps B27 allospecificity to the region around position 70 in the alpha 1 domain.

作者信息

Choo S Y, Fan L A, Hansen J A

机构信息

Fred Hutchinson Cancer Research Center, Seattle, WA 98104.

出版信息

J Immunol. 1991 Jul 1;147(1):174-80.

PMID:1711072
Abstract

There are six known HLA-B alleles that share the HLA-B27 allospecificity, yet differ by one to six amino acid substitutions. Each of these B27 alleles can be readily assigned by one of the six representative IEF patterns. Two unrelated individuals, LH and HS, express B27 Ag that appear to be identical by IEF, but an HLA-B27 alloreactive CTL clone I-73 was found to react differently with these cells, suggesting these B27 molecules are not identical. We sequenced polymerase chain reaction-amplified B27 cDNA clones obtained from HS and compared its deduced amino acid sequence (B27-HS) with the B27 sequence of LH (B27-LH) which was previously designated the B*2701 allele. B27-HS and B27-LH differ by eight amino acids; three in alpha 1 domain and five in alpha 2 domain. These amino acid substitutions of B27-HS altered T cell recognition but not the B27 serologic epitope or IEF pattern. B27-HS differs from the six known B27 alleles by five to eight amino acid substitutions, and thus it represents the seventh allele of the HLA-B27 Ag family. This novel B27 allele might have been derived from a gene conversion event. Previously, two amino acid residues at positions 70 and 97 were suggested to be specific for B27 Ag family. B27-HS now reveals that Lys at position 70 is specific for B27 but Asn at position 97 is not. We propose that the region around position 70 might be crucial in determining the B27 serologic epitope and possibly in peptide Ag binding. This study also demonstrates that class I molecules of the same Ag specificity sharing an indistinguishable IEF pattern are not necessarily identical, and indicates that only the definitive determination of primary structure would identify all the class I alleles that are functionally relevant in regard to alloreactivity, T cell restriction, and disease association.

摘要

已知有六种HLA - B等位基因具有HLA - B27同种特异性,但它们之间存在一到六个氨基酸的替换差异。这些B27等位基因中的每一个都可以通过六种代表性的IEF模式之一轻松识别。两个不相关的个体LH和HS,通过IEF检测显示其表达的B27抗原似乎相同,但发现一个HLA - B27同种反应性CTL克隆I - 73与这些细胞的反应不同,这表明这些B27分子并不相同。我们对从HS获得的聚合酶链反应扩增的B27 cDNA克隆进行了测序,并将其推导的氨基酸序列(B27 - HS)与LH的B27序列(B27 - LH,先前被指定为B*2701等位基因)进行了比较。B27 - HS和B27 - LH有八个氨基酸不同;α1结构域中有三个,α2结构域中有五个。B27 - HS的这些氨基酸替换改变了T细胞识别,但没有改变B27血清学表位或IEF模式。B27 - HS与六种已知的B27等位基因有五到八个氨基酸替换差异,因此它代表了HLA - B27抗原家族的第七个等位基因。这个新的B27等位基因可能源自基因转换事件。此前,有人提出70位和97位的两个氨基酸残基是B27抗原家族所特有的。现在B27 - HS显示70位的赖氨酸是B27所特有的,但97位的天冬酰胺不是。我们提出70位附近的区域可能在决定B27血清学表位以及可能在肽抗原结合方面至关重要。这项研究还表明,具有难以区分的IEF模式的相同抗原特异性的I类分子不一定相同,并表明只有一级结构的明确确定才能识别所有在同种反应性、T细胞限制性和疾病关联方面具有功能相关性的I类等位基因。

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