4.7 Article

Mechanosensing machinery for cells under low substratum rigidity

Journal

AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volume 295, Issue 6, Pages C1579-C1589

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajpcell.00223.2008

Keywords

focal adhesion kinase; beta(1)-integrin activation; beta(1)-integrin clustering; lipid raft; actin cytoskeleton

Funding

  1. National Health Research Institute [NHRI-EX95-9430SI]
  2. National Science Council, ROC [95-2120-M-006-007]

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Wei WC, Lin HH, Shen MR, Tang MJ. Mechanosensing machinery for cells under low substratum rigidity. Am J Physiol Cell Physiol 295: C1579-C1589, 2008. First published October 15, 2008; doi:10.1152/ajpcell.00223.2008.-Mechanical stimuli are essential during development and tumorigenesis. However, how cells sense their physical environment under low rigidity is still unknown. Here we show that low rigidity of collagen gel downregulates beta(1)-integrin activation, clustering, and focal adhesion kinase (FAK) Y397 phosphorylation, which is mediated by delayed raft formation. Moreover, overexpression of autoclustered beta(1)-integrin (V737N), but not constitutively active beta(1)-integrin (G429N), rescues FAKY397 phosphorylation level suppressed by low substratum rigidity. Using fluorescence resonance energy transfer to assess beta(1)-integrin clustering, we have found that substratum rigidity between 58 and 386 Pa triggers beta(1)-integrin clustering in a dose-dependent manner, which is highly dependent on actin filaments but not microtubules. Furthermore, augmentation of beta(1)-integrin clustering enhances the interaction between beta(1)-integrin, FAK, and talin. Our results indicate that contact with collagen fibrils is not sufficient for integrin activation. However, substratum rigidity is required for integrin clustering and activation. Together, our findings provide new insight into the mechanosensing machinery and the mode of action for epithelial cells in response to their physical environment under low rigidity.

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