期刊
JOURNAL OF CELL BIOLOGY
卷 187, 期 5, 页码 715-731出版社
ROCKEFELLER UNIV PRESS
DOI: 10.1083/jcb.200908134
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资金
- Swiss National Science Foundation [3100AO-103805]
- Nevus Outreach, Inc.
- Swiss Foundation for Research on Myopathies
- French Association for Cancer Research
- French Foundation for Medical Research
- European Molecular Biology Organization
- Academy of Finland
- Fund for Scientific Research-Flanders
- Interuniversity Attraction Poles of the Prime Ministers Services
- Belgian Federation against Cancer
- Catholic University Leuven
Integrin-dependent adhesion sites consist of clustered integrins that transmit mechanical forces and provide signaling required for cell survival and morphogenesis. Despite their importance, the regulation of integrin clustering by the cytoplasmic adapter protein talin (Tal) and phosphatidylinositol (PI)-4,5-biphosphate (PI(4,5)P-2) lipids nor their dynamic coupling to the actin cytoskeleton is fully understood. By using a Tal-dependent integrin clustering assay in intact cells, we identified a PI(4,5)P-2-binding basic ridge spanning across the F2 and F3 domains of the Tal head that regulates integrin clustering. Clustering requires a new PI(4,5)P-2-binding site in F2 and is negatively regulated by autoinhibitory interactions between F3 and the Tal rod (Tal-R). The release of the Tal-R exposes a new beta 3-integrin-binding site in F3, enabling interaction with a membrane proximal acidic motif, which involves the formation of salt bridges between K-316 and K-324 with E-726 and D-723, respectively. This interaction shields the beta-integrin tail from reassociation with its beta subunit, thereby maintaining the integrin in a substrate-binding and clustering-competent form.
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