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来自MHC I类缺陷小鼠的自然杀伤细胞上Ly49抑制性受体的表达改变。

Altered expression of Ly49 inhibitory receptors on natural killer cells from MHC class I-deficient mice.

作者信息

Salcedo M, Diehl A D, Olsson-Alheim M Y, Sundbäck J, Van Kaer L, Kärre K, Ljunggren H G

机构信息

Microbiology and Tumor Biology Center, Karolinska Institute, Stockholm, Sweden.

出版信息

J Immunol. 1997 Apr 1;158(7):3174-80.

PMID:9120271
Abstract

MHC class I molecules in the host affect the specificity of NK cells. Previous work has suggested that this specificity is conferred by the expression of products encoded by the Ly49 gene family. This gene family encodes receptors that upon specific recognition of MHC class I ligands mediate an inhibitory signal that prevents killing by NK cells. The pattern of expression of the Ly49 MHC class I binding inhibitory receptors on NK cells is thought to be adapted to the host to ensure the generation of a self-tolerant, yet functional, NK cell repertoire. In the present study we have examined the expression of inhibitory receptors (Ly49A, Ly49C, and Ly49G2) on NK1.1+ cells from B6 (H-2b) and D8 (B6 mice transgenic for H-2Dd) mice as well as corresponding TAP1 -/-, beta2m -/-, and TAP1/beta2m -/- mutants of these mice. We demonstrate that receptor expression on NK1.1+ cells can be specifically modulated by host MHC class I molecules in at least two different ways: alteration of numbers of cells expressing a given receptor and modulation of the levels of expression of a given receptor at the cell surface. The degree of this modulation varies significantly among the various receptors studied and may depend upon the nature of their MHC class I ligands. The results are discussed in relation to the influence of MHC class I molecules on the development of an NK cell repertoire.

摘要

宿主中的MHC I类分子会影响自然杀伤细胞(NK细胞)的特异性。此前的研究表明,这种特异性是由Ly49基因家族编码的产物的表达所赋予的。该基因家族编码的受体在特异性识别MHC I类配体后,介导一种抑制性信号,可阻止NK细胞的杀伤作用。NK细胞上Ly49 MHC I类结合抑制性受体的表达模式被认为是适应宿主的,以确保产生一个自我耐受但仍具功能的NK细胞库。在本研究中,我们检测了来自B6(H-2b)和D8(转H-2Dd基因的B6小鼠)小鼠以及这些小鼠相应的TAP1 -/-、β2m -/-和TAP1/β2m -/-突变体的NK1.1+细胞上抑制性受体(Ly49A、Ly49C和Ly49G2)的表达。我们证明,NK1.1+细胞上的受体表达可通过至少两种不同方式被宿主MHC I类分子特异性调节:改变表达特定受体的细胞数量以及调节细胞表面特定受体的表达水平。这种调节程度在所研究的各种受体之间存在显著差异,并且可能取决于它们MHC I类配体的性质。我们结合MHC I类分子对NK细胞库发育的影响对这些结果进行了讨论。

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