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肽决定了抗原呈递细胞中MHC II类分子的寿命。

Peptides determine the lifespan of MHC class II molecules in the antigen-presenting cell.

作者信息

Nelson C A, Petzold S J, Unanue E R

机构信息

Center for Immunology, Washington University School of Medicine, St Louis, Missouri 63110.

出版信息

Nature. 1994 Sep 15;371(6494):250-2. doi: 10.1038/371250a0.

Abstract

Although many peptides are generated during the intracellular processing of protein antigens, only a few are selected for recognition by the immune system. The immunodominant epitope of hen egg white lysozyme (HEL) for H-2k mice is contained in a tryptic fragment of amino-acid residues 46-61 (refs 6, 7). The core of this T-cell epitope, from amino acids 52 to 61 (DYGILQINSR), contains those residues required for binding to the class II molecule I-Ak (ref. 7). Most of the naturally processed fragments recovered from I-Ak-bearing antigen-presenting cells (APCs) cultured with HEL contained this 52-61 core sequence, presented as a nested set of peptides with extensions at both the amino and carboxyl termini. We now compare the handling by APCs of peptides containing HEL 52-61 to establish whether there is an advantage for the APC in selecting extended peptides: different complexes between peptides and major histocompatibility complex (MHC) molecules varied greatly in the amount of time associated with the APC, and in their immunogenic strength. This difference in persistence is one of the factors contributing to the selection and immune recognition of peptide-MHC complexes by T cells.

摘要

尽管在蛋白质抗原的细胞内加工过程中会产生许多肽段,但只有少数被免疫系统选中以供识别。对于H-2k小鼠而言,鸡蛋清溶菌酶(HEL)的免疫显性表位包含在氨基酸残基46 - 61的胰蛋白酶片段中(参考文献6、7)。这个T细胞表位的核心,即氨基酸52至61(DYGILQINSR),包含与II类分子I-Ak结合所需的那些残基(参考文献7)。从用HEL培养的携带I-Ak的抗原呈递细胞(APC)中回收的大多数天然加工片段都包含这个52 - 61核心序列,呈现为一组嵌套的肽段,在氨基和羧基末端都有延伸。我们现在比较APC对含有HEL 52 - 61的肽段的处理情况,以确定APC在选择延伸肽段方面是否具有优势:肽段与主要组织相容性复合体(MHC)分子之间的不同复合物与APC相关联的时间量以及它们的免疫原性强度差异很大。这种持久性的差异是促成T细胞对肽-MHC复合物进行选择和免疫识别的因素之一。

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