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RNA干扰文库筛选揭示Gβ1、酪蛋白激酶2和ICAP-1是LFA-1介导的T细胞极性和迁移的新型调节因子。

RNAi library screening reveals Gβ1, Casein Kinase 2 and ICAP-1 as novel regulators of LFA-1-mediated T cell polarity and migration.

作者信息

Haap-Hoff Antje, Freeley Michael, Dempsey Eugene, Dunican Dara, Bennett Emily, Triglia Denise, Skubis-Zegadlo Joanna, Mitchell Davies Anthony, Kelleher Dermot, Long Aideen

机构信息

Trinity Translational Medicine Institute & Department of Clinical Medicine, Trinity College Dublin, St James's Hospital, Dublin, Republic of Ireland.

出版信息

Immunol Cell Biol. 2025 Jan;103(1):73-92. doi: 10.1111/imcb.12838. Epub 2024 Nov 28.

DOI:10.1111/imcb.12838
PMID:39607284
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11688611/
Abstract

The αβ integrin LFA-1 plays a key role in T-cell adhesion to the endothelial vasculature and migration into both secondary lymphoid organs and peripheral tissues via interactions with its target protein ICAM-1, but the pathways that regulate LFA-1-mediated T-cell polarity and migration are not fully understood. In this study we screened two RNAi libraries targeting G protein-coupled receptors (GPCR)/GPCR-associated proteins and kinases in a HuT 78 T cell line model of LFA-1-stimulated T-cell migration. Based on staining of the actin cytoskeleton, multiple parameters to measure cell morphology were used to assess the contribution of 1109 genes to LFA-1-mediated T-cell polarity and migration. These RNAi screens identified a number of both novel and previously identified genes that either increased or decreased the polarity and migratory capacity of these cells. Following multiparametric analysis, hierarchical clustering and pathway analysis, three of these genes were characterized in further detail using primary human T cells, revealing novel roles for the heterotrimeric G protein subunit Gβ1 and Casein Kinase 2 in LFA-1-mediated T-cell polarity and migration in vitro. Our studies also highlighted a new role for ICAP-1, an adaptor protein previously described to be associated with β1 integrins, in β2 integrin LFA-1-directed migration in T cells. Knockdown of ICAP-1 expression in primary T cells revealed a role in cell polarity, cell velocity and transmigration towards SDF-1 for this adaptor protein. This study therefore uncovers new roles for GPCR/GPCR-associated proteins and kinases in T-cell migration and provides potential novel targets for modulation of the T-cell immune response.

摘要

αβ整合素淋巴细胞功能相关抗原-1(LFA-1)通过与其靶蛋白细胞间黏附分子-1(ICAM-1)相互作用,在T细胞与内皮血管系统的黏附以及向次级淋巴器官和外周组织的迁移中发挥关键作用,但调节LFA-1介导的T细胞极性和迁移的途径尚未完全明确。在本研究中,我们在LFA-1刺激的T细胞迁移的HuT 78 T细胞系模型中筛选了两个靶向G蛋白偶联受体(GPCR)/GPCR相关蛋白和激酶的RNA干扰文库。基于肌动蛋白细胞骨架的染色,使用多个测量细胞形态的参数来评估1109个基因对LFA-1介导的T细胞极性和迁移的作用。这些RNA干扰筛选鉴定出了一些新的和先前已鉴定的基因,它们要么增加要么降低了这些细胞的极性和迁移能力。经过多参数分析、层次聚类和通路分析后,使用原代人T细胞对其中三个基因进行了更详细的表征,揭示了异源三聚体G蛋白亚基Gβ1和酪蛋白激酶2在体外LFA-1介导的T细胞极性和迁移中的新作用。我们的研究还突出了ICAP-1(一种先前描述为与β1整合素相关的衔接蛋白)在T细胞中β2整合素LFA-1导向的迁移中的新作用。在原代T细胞中敲低ICAP-1的表达揭示了该衔接蛋白在细胞极性、细胞速度和向基质细胞衍生因子-1(SDF-1)迁移方面的作用。因此,本研究揭示了GPCR/GPCR相关蛋白和激酶在T细胞迁移中的新作用,并为调节T细胞免疫反应提供了潜在的新靶点。

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