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pTRAPs:固有免疫信号传导中的跨膜衔接蛋白

pTRAPs: Transmembrane adaptors in innate immune signaling.

作者信息

Curson James E B, Luo Lin, Sweet Matthew J, Stow Jennifer L

机构信息

Institute for Molecular Bioscience (IMB), IMB Centre for Inflammation and Disease Research and Australian Infectious Diseases Research Centre, The University of Queensland, Brisbane, Queensland, Australia.

出版信息

J Leukoc Biol. 2018 Mar 30. doi: 10.1002/JLB.2RI1117-474R.

Abstract

Transmembrane adaptor proteins (TRAPs) are protein scaffolds and signaling regulators with established roles in signal-induced activation of lymphocytes. A subset of the TRAP family, the palmitoylated TRAPs (pTRAPs), are increasingly emerging with additional roles in innate immune cells. Targeted to lipid rafts, tetraspannin-enriched microdomains, and protein microclusters in membranes, pTRAP scaffolds exert spatiotemporal regulation by recruiting signaling kinases, particularly Src and Syk family members, as well as Csk, and other effectors. In this way, pTRAPs modulate signaling and influence resulting cell responses, including the selective output of inflammatory cytokines and other mediators. Here, we review studies revealing that different pTRAPs work together, often with overlapping or redundant roles, for positive and negative regulation of key innate immune pathways, including Fc receptor and pattern recognition receptor signaling. Recent findings show that pTRAPs can bind directly to innate immune receptors, in addition to other transmembrane binding partners. Thus, pTRAPs are important, multifunctional scaffolds in pathways that are fundamental to diverse innate immune responses.

摘要

跨膜衔接蛋白(TRAPs)是蛋白质支架和信号调节剂,在淋巴细胞的信号诱导激活中发挥既定作用。TRAP家族的一个亚群,即棕榈酰化TRAPs(pTRAPs),在先天免疫细胞中发挥的其他作用日益显现。pTRAP支架定位于脂筏、富含四跨膜蛋白的微结构域和膜中的蛋白质微簇,通过招募信号激酶,特别是Src和Syk家族成员以及Csk和其他效应器来发挥时空调节作用。通过这种方式,pTRAPs调节信号传导并影响由此产生的细胞反应,包括炎性细胞因子和其他介质的选择性输出。在此,我们综述了相关研究,这些研究表明不同的pTRAPs协同发挥作用,其作用通常重叠或冗余,对包括Fc受体和模式识别受体信号传导在内的关键先天免疫途径进行正调控和负调控。最近的研究结果表明,除了其他跨膜结合伙伴外,pTRAPs还可以直接与先天免疫受体结合。因此,pTRAPs是多种先天免疫反应所必需的途径中的重要多功能支架。

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