Structural Basis of Human Full-length Kindlin-3 Homotrimer in an Auto-inhibited State

Overview

Journal PLoS Biol

Specialty Biology

Date 2020 Jul 10

PMID 32644996

Citations 20

Authors

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

Affiliations

Soon will be listed here.

Abstract

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.

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