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T细胞受体(TCR)与半抗原的相互作用:金属离子作为非经典半抗原。

T cell receptor (TCR) interaction with haptens: metal ions as non-classical haptens.

作者信息

Thierse Hermann-Josef, Gamerdinger Katharina, Junkes Christof, Guerreiro Nelson, Weltzien Hans Ulrich

机构信息

Max-Planck-Institut für Immunbiologie, Stübeweg 51, D-79108 Freiburg, Germany.

出版信息

Toxicology. 2005 Apr 15;209(2):101-7. doi: 10.1016/j.tox.2004.12.015. Epub 2005 Jan 23.

Abstract

Haptens are classified as low molecular chemicals with an intrinsic potential to covalently modify proteins, and many of them are strong inducers of contact hypersensitivity (CHS). CHS is T cell mediated, and hapten-specific T cells have been shown to interact with hapten-modified, MHC-associated peptides. However, the most common contact sensitizer in the industrialized world is nickel. In contrast to classical haptens, nickel ions do not form covalent bonds to proteins, but rather become caught in reversible coordination complexes. We here review work demonstrating that some T cells, indeed, may react to such Ni complexes on the MHC/peptide-surface absolutely comparable to other haptens. In other cases, Ni ions unlike classical haptens, may activate T cells by crosslinking their receptors to MHC molecules, independent of the nature of the associated peptide. Moreover, Ni-interacting proteins appear to make use of the reversibility of Ni-binding, and to mediate the transfer of Ni-ions to the receptor-MHC interphase. We have demonstrated such properties for human serum albumin (HSA) as well as for transferrin and identified numerous new Ni-binding proteins in human B-cell lines or dendritic cells by affinity purification and mass spectroscopy. These proteins include a notable number of known heat shock proteins and chaperones, implying that Ni may functionally interfere with these stress proteins.

摘要

半抗原被归类为具有共价修饰蛋白质内在潜力的低分子化学物质,其中许多是接触性超敏反应(CHS)的强诱导剂。CHS是由T细胞介导的,并且已证明半抗原特异性T细胞可与半抗原修饰的、与主要组织相容性复合体(MHC)相关的肽相互作用。然而,工业化世界中最常见的接触性致敏剂是镍。与经典半抗原不同,镍离子不会与蛋白质形成共价键,而是形成可逆的配位络合物。我们在此综述了一些研究工作,这些研究表明,一些T细胞确实可能对半抗原与MHC/肽表面上的此类镍络合物产生反应,这与其他半抗原完全可比。在其他情况下,与经典半抗原不同,镍离子可能通过将其受体与MHC分子交联来激活T细胞,而与相关肽的性质无关。此外,与镍相互作用的蛋白质似乎利用了镍结合的可逆性,并介导镍离子向受体 - MHC界面的转移。我们已经证明了人血清白蛋白(HSA)以及转铁蛋白具有此类特性,并通过亲和纯化和质谱法在人B细胞系或树突状细胞中鉴定了许多新的镍结合蛋白。这些蛋白质包括大量已知的热休克蛋白和伴侣蛋白,这意味着镍可能在功能上干扰这些应激蛋白。

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