4.5 Article

The LIM Domain of Zyxin Is Sufficient for Force-Induced Accumulation of Zyxin During Cell Migration

期刊

BIOPHYSICAL JOURNAL
卷 101, 期 5, 页码 1069-1075

出版社

CELL PRESS
DOI: 10.1016/j.bpj.2011.08.001

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资金

  1. Beckman Young Investigator Award
  2. Hellman Family New Faculty Award
  3. National Institutes of Health [T32-GM08799]
  4. University of California Cancer Research Coordinating Committee
  5. Achievement Rewards for College Scientists Award

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Cellular responses to mechanical perturbation are vital to cell physiology. In particular, migrating cells have been shown to sense substrate stiffness and alter cell morphology and speed. Zyxin is a focal adhesion protein that responds to external mechanical forces; however, the mechanisms of zyxin recruitment at force-bearing sites are unknown. Using force-sensing microfabricated substrates, we simultaneously measured traction force and zyxin recruitment at force-bearing sites. GFP-tagged zyxin accumulates at force-bearing sites at the leading edge, but not at the trailing edge, of migrating epithelial cells. Zyxin recruitment at force-bearing sites depends on Rho-kinase and myosin II activation, suggesting that zyxin responds not only to the externally applied force, as previously shown, but also to the internally generated actin-myosin force. Zyxin in turn recruits vasodilator-stimulated phosphoprotein, a regulator of actin assembly, to force-bearing sites. To dissect the domains of zyxin that are essential for this unique force-dependent accumulation, we generated two zyxin truncation mutants: one lacking the LIM domain (Delta LIM) and one containing only the LIM domain with all three LIM motifs (LIM). GFP-tagged Delta LIM does not localize to the force-bearing sites, but GFP-tagged zyxin LIM-domain is sufficient for the recruitment to and dynamics at force-bearing focal adhesions. Furthermore, one or two LIM motifs are not sufficient for force-dependent accumulation, suggesting that all three LIM motifs are required. Therefore, the LIM domain of zyxin recruits zyxin to force-bearing sites at the leading edge of migrating cells.

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