与信号蛋白的选择性关联决定了NKG2D的刺激活性与共刺激活性。

Selective associations with signaling proteins determine stimulatory versus costimulatory activity of NKG2D.

作者信息

Diefenbach Andreas, Tomasello Elena, Lucas Mathias, Jamieson Amanda M, Hsia Jennifer K, Vivier Eric, Raulet David H

机构信息

Department of Molecular and Cell Biology and Cancer Research Laboratory, University of California, Berkeley, CA 94720-3200, USA.

出版信息

Nat Immunol. 2002 Dec;3(12):1142-9. doi: 10.1038/ni858. Epub 2002 Nov 11.

DOI:10.1038/ni858

PMID:12426565

Abstract

Optimal lymphocyte activation requires the simultaneous engagement of stimulatory and costimulatory receptors. Stimulatory immunoreceptors are usually composed of a ligand-binding transmembrane protein and noncovalently associated signal-transducing subunits. Here, we report that alternative splicing leads to two distinct NKG2D polypeptides that associate differentially with the DAP10 and KARAP (also known as DAP12) signaling subunits. We found that differential expression of these isoforms and of signaling proteins determined whether NKG2D functioned as a costimulatory receptor in the adaptive immune system (CD8+ T cells) or as both a primary recognition structure and a costimulatory receptor in the innate immune system (natural killer cells and macrophages). This strategy suggests a rationale for the multisubunit structure of stimulatory immunoreceptors.

摘要

最佳的淋巴细胞激活需要刺激受体和共刺激受体同时参与。刺激免疫受体通常由一个配体结合跨膜蛋白和非共价结合的信号转导亚基组成。在此，我们报道可变剪接导致两种不同的NKG2D多肽，它们与DAP10和KARAP（也称为DAP12）信号亚基的结合方式不同。我们发现这些异构体和信号蛋白的差异表达决定了NKG2D在适应性免疫系统（CD8 + T细胞）中作为共刺激受体，还是在先天性免疫系统（自然杀伤细胞和巨噬细胞）中作为主要识别结构和共刺激受体发挥作用。这一策略为刺激免疫受体的多亚基结构提供了一种理论依据。

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与信号蛋白的选择性关联决定了NKG2D的刺激活性与共刺激活性。

Selective associations with signaling proteins determine stimulatory versus costimulatory activity of NKG2D.

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