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识别自身主要组织相容性复合体分子的T细胞独特型:H-2特异性、同种异型连锁以及在功能性T细胞群体上的表达

T cell idiotypes recognizing self-major histocompatibility complex molecules: H-2 specificity, allotype linkage, and expression on functional T cell populations.

作者信息

Nagy Z A, Elliott B E, Carlow D A, Rubin B

出版信息

Eur J Immunol. 1982 May;12(5):393-400. doi: 10.1002/eji.1830120507.

Abstract

An anti-idiotypic serum (antiserum 5936, B. Rubin et al., J. Exp. Med. 1979. 150: 307) was used to demonstrate receptor sites for self-major histocompatibility complex (MHC) antigens on T lymphocytes. The antiserum was raised by injecting rabbits tolerant to mouse Ig with a B6 anti-CBA (anti-H2k) alloantibody. It recognized a large proportion of T cells from H-2k strains carrying the b, c, d or e allele at the Igh-1 locus, but only a few T cells from H-2k strains with Igh-1 alleles a, f and j. Allotype linkage of the 5936 idiotype was also demonstrated by segregation analysis. The antiserum did not recognize either H-2k B cells or T cells from other H-2 haplotypes despite the presence of a permissive Igh-1 allele. The 5936 idiotype was found to be associated with several different antigen specificities, indicating that it is not located on the binding site for foreign antigen. Furthermore, the 5936 antiserum inhibited the binding of soluble Ik antigens by H-2k, Igh-1b, T cells, and, in the presence of complement, eliminated T cells responding to different antigens in an I-Ak-restricted fashion. Collectively, the data indicate that the structure bearing the 5936 idiotype is a receptor for I-Ak antigens, expressed by strains carrying the I-Ak allele and a permissive allele at the Igh-1 locus. The relevance of this finding to the MHC-restricted recognition of antigens by T cells is discussed.

摘要

一种抗独特型血清(抗血清5936,B.鲁宾等人,《实验医学杂志》1979年。150:307)被用于证明T淋巴细胞上自身主要组织相容性复合体(MHC)抗原的受体位点。该抗血清是通过用B6抗CBA(抗H2k)同种异体抗体注射对小鼠Ig耐受的兔子而产生的。它识别来自Igh-1位点携带b、c、d或e等位基因的H-2k品系的大部分T细胞,但只识别来自Igh-1等位基因为a、f和j的H-2k品系的少数T细胞。通过分离分析也证明了5936独特型的同种异型连锁。尽管存在允许的Igh-1等位基因,该抗血清既不识别H-2k B细胞,也不识别来自其他H-2单倍型的T细胞。发现5936独特型与几种不同的抗原特异性相关,这表明它不位于外来抗原的结合位点上。此外,5936抗血清抑制了H-2k、Igh-1b、T细胞对可溶性Ik抗原的结合,并且在补体存在的情况下,消除了以I-Ak限制方式对不同抗原作出反应的T细胞。总体而言,数据表明带有5936独特型的结构是I-Ak抗原的受体,由在Igh-1位点携带I-Ak等位基因和允许等位基因的品系表达。讨论了这一发现与T细胞对MHC限制的抗原识别的相关性。

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