Literature DB >> 33058779

Mechanosensing through Direct Binding of Tensed F-Actin by LIM Domains.

Xiaoyu Sun1, Donovan Y Z Phua1, Lucas Axiotakis2, Mark A Smith3, Elizabeth Blankman3, Rui Gong1, Robert C Cail2, Santiago Espinosa de Los Reyes1, Mary C Beckerle3, Clare M Waterman4, Gregory M Alushin5.   

Abstract

Mechanical signals transmitted through the cytoplasmic actin cytoskeleton must be relayed to the nucleus to control gene expression. LIM domains are protein-protein interaction modules found in cytoskeletal proteins and transcriptional regulators. Here, we identify three LIM protein families (zyxin, paxillin, and FHL) whose members preferentially localize to the actin cytoskeleton in mechanically stimulated cells through their tandem LIM domains. A minimal actin-myosin reconstitution system reveals that representatives of all three families directly bind F-actin only in the presence of mechanical force. Point mutations at a site conserved in each LIM domain of these proteins disrupt tensed F-actin binding in vitro and cytoskeletal localization in cells, demonstrating a common, avidity-based mechanism. Finally, we find that binding to tensed F-actin in the cytoplasm excludes the cancer-associated transcriptional co-activator FHL2 from the nucleus in stiff microenvironments. This establishes direct force-activated F-actin binding as a mechanosensing mechanism by which cytoskeletal tension can govern nuclear localization.
Copyright © 2020 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  FHL2; LIM domain; actin; cytoskeleton; mechanobiology; mechanosensation; mechanotransduction; paxillin; zyxin

Year:  2020        PMID: 33058779      PMCID: PMC7686152          DOI: 10.1016/j.devcel.2020.09.022

Source DB:  PubMed          Journal:  Dev Cell        ISSN: 1534-5807            Impact factor:   12.270


  69 in total

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