PLoS Biology (Jul 2020)

Structural basis of human full-length kindlin-3 homotrimer in an auto-inhibited state.

  • Wenting Bu,
  • Zarina Levitskaya,
  • Zhi Yang Loh,
  • Shengyang Jin,
  • Shibom Basu,
  • Rya Ero,
  • Xinfu Yan,
  • Meitian Wang,
  • So Fong Cam Ngan,
  • Siu Kwan Sze,
  • Suet-Mien Tan,
  • Yong-Gui Gao

DOI
https://doi.org/10.1371/journal.pbio.3000755
Journal volume & issue
Vol. 18, no. 7
p. e3000755

Abstract

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Kindlin-1, -2, and -3 directly bind integrin β cytoplasmic tails to regulate integrin activation and signaling. Despite their functional significance and links to several diseases, structural information on full-length kindlin proteins remains unknown. Here, we report the crystal structure of human full-length kindlin-3, which reveals a novel homotrimer state. Unlike kindlin-3 monomer, which is the major population in insect and mammalian cell expression systems, kindlin-3 trimer does not bind integrin β cytoplasmic tail as the integrin-binding pocket in the F3 subdomain of 1 protomer is occluded by the pleckstrin homology (PH) domain of another protomer, suggesting that kindlin-3 is auto-inhibited upon trimer formation. This is also supported by functional assays in which kindlin-3 knockout K562 erythroleukemia cells reconstituted with the mutant kindlin-3 containing trimer-disrupting mutations exhibited an increase in integrin-mediated adhesion and spreading on fibronectin compared with those reconstituted with wild-type kindlin-3. Taken together, our findings reveal a novel mechanism of kindlin auto-inhibition that involves its homotrimer formation.