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嵌合II类/I类主要组织相容性复合体分子的T细胞识别及L3T4的作用

T-cell recognition of a chimaeric class II/class I MHC molecule and the role of L3T4.

作者信息

Golding H, McCluskey J, Munitz T I, Germain R N, Margulies D H, Singer A

出版信息

Nature. 1985;317(6036):425-7. doi: 10.1038/317425a0.

Abstract

In addition to expressing clonally distributed antigen-specific and major histocompatibility complex (MHC)-restricted receptors, T cells also express non-clonally distributed surface molecules that are involved in T-cell function. Among the most intriguing of the latter are L3T4 and Lyt 2, which are expressed on individual T lymphocytes in striking, though not absolute, concordance with their restriction by either class II or class I MHC determinants, and which are thought to contribute to the overall avidity of T-cell interactions by binding to monomorphic determinants on class II and class I MHC molecules, respectively. To examine the ability of T cells to recognize a single class II domain in the absence of the remainder of the Ia molecule, as well as to evaluate the structural basis for the putative interaction of L3T4 with Ia, a recombinant class II/class I murine MHC gene was constructed and introduced into mouse L cells. Here we demonstrate that a subset of class II allospecific cytotoxic T lymphocytes (CTL) can specifically recognize and lyse L-cell transfectants expressing an isolated polymorphic A beta 1 domain, and that anti-L3T4 antibody can block such killing, a result inconsistent with the highly conserved membrane-proximal domains of Ia acting as unique target sites for L3T4 binding.

摘要

除了表达克隆分布的抗原特异性和主要组织相容性复合体(MHC)限制性受体外,T细胞还表达参与T细胞功能的非克隆分布的表面分子。其中最引人关注的是L3T4和Lyt 2,它们在单个T淋巴细胞上表达,与它们受II类或I类MHC决定簇的限制呈现出显著(尽管不是绝对)的一致性,并且被认为分别通过与II类和I类MHC分子上的单态决定簇结合,对T细胞相互作用的总体亲和力有贡献。为了研究T细胞在没有Ia分子其余部分的情况下识别单个II类结构域的能力,以及评估L3T4与Ia假定相互作用的结构基础,构建了一个重组II类/I类小鼠MHC基因并将其导入小鼠L细胞。在此我们证明,一部分II类同种异体特异性细胞毒性T淋巴细胞(CTL)能够特异性识别并裂解表达分离的多态性Aβ1结构域的L细胞转染子,并且抗L3T4抗体能够阻断这种杀伤作用,这一结果与Ia高度保守的膜近端结构域作为L3T4结合的独特靶位点不一致。

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