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T细胞利用粘着斑在受限环境中拉动自身前进。

T cells Use Focal Adhesions to Pull Themselves Through Confined Environments.

作者信息

Caillier Alexia, Oleksyn David, Fowell Deborah J, Miller Jim, Oakes Patrick W

机构信息

Department of Cell & Molecular Physiology, Loyola University Chicago, Stritch School of Medicine, Maywood, IL 60153, USA.

David H. Smith Center for Vaccine Biology and Immunology, Aab Institute of Biomedical Sciences, Department of Microbiology and Immunology, University of Rochester Medical Center, Rochester, NY 14642, USA.

出版信息

bioRxiv. 2023 Oct 19:2023.10.16.562587. doi: 10.1101/2023.10.16.562587.

Abstract

Immune cells are highly dynamic and able to migrate through environments with diverse biochemical and mechanical composition. Their migration has classically been defined as amoeboid under the assumption that it is integrin-independent. Here we show that activated primary Th1 T cells require both confinement and extracellular matrix protein to migrate efficiently. This migration is mediated through small and dynamic focal adhesions that are composed of the same proteins associated with canonical mesenchymal focal adhesions, such as integrins, talin, and vinculin. These focal adhesions, furthermore, localize to sites of contractile traction stresses, enabling T cells to pull themselves through confined spaces. Finally, we show that Th1 T cell preferentially follows tracks of other T cells, suggesting that these adhesions are modifying the extracellular matrix to provide additional environmental guidance cues. These results demonstrate not only that the boundaries between amoeboid and mesenchymal migration modes are ambiguous, but that integrin-mediated adhesions play a key role in T cell motility.

摘要

免疫细胞具有高度的动态性,能够在具有不同生化和机械组成的环境中迁移。传统上,它们的迁移被定义为阿米巴样迁移,其假设是不依赖整合素。在这里,我们表明活化的原代Th1 T细胞需要受限环境和细胞外基质蛋白才能有效迁移。这种迁移是通过小的动态黏着斑介导的,这些黏着斑由与典型间充质黏着斑相关的相同蛋白质组成,如整合素、踝蛋白和纽蛋白。此外,这些黏着斑定位于收缩牵引应力部位,使T细胞能够在受限空间中拉动自身。最后,我们表明Th1 T细胞优先沿着其他T细胞的轨迹移动,这表明这些黏附正在修饰细胞外基质,以提供额外的环境引导线索。这些结果不仅表明阿米巴样迁移模式和间充质迁移模式之间的界限是模糊的,而且整合素介导的黏附在T细胞运动中起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/21fb/10614902/33f009d7a9d8/nihpp-2023.10.16.562587v1-f0002.jpg

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