Excitable Rho dynamics control cell shape and motility by sequentially activating ERM proteins and actomyosin contractility

Author:

Marshall-Burghardt Seph12ORCID,Migueles-Ramírez Rodrigo A.13ORCID,Lin Qiyao12ORCID,El Baba Nada12ORCID,Saada Rayan1,Umar Mustakim1ORCID,Mavalwala Kian1ORCID,Hayer Arnold1ORCID

Affiliation:

1. Department of Biology, Stewart Biology Building, McGill University, Montréal, Québec H3A 1B1, Canada.

2. Graduate Program in Biology, McGill University, Montréal, Québec, Canada.

3. PhD Program in Quantitative Life Sciences, McGill University, Montréal, Québec, Canada.

Abstract

Migration of endothelial and many other cells requires spatiotemporal regulation of protrusive and contractile cytoskeletal rearrangements that drive local cell shape changes. Unexpectedly, the small GTPase Rho, a crucial regulator of cell movement, has been reported to be active in both local cell protrusions and retractions, raising the question of how Rho activity can coordinate cell migration. Here, we show that Rho activity is absent in local protrusions and active during retractions. During retractions, Rho rapidly activated ezrin-radixin-moesin proteins (ERMs) to increase actin-membrane attachment, and, with a delay, nonmuscle myosin 2 (NM2). Rho activity was excitable, with NM2 acting as a slow negative feedback regulator. Strikingly, inhibition of SLK/LOK kinases, through which Rho activates ERMs, caused elongated cell morphologies, impaired Rho-induced cell contractions, and reverted Rho-induced blebbing. Together, our study demonstrates that Rho activity drives retractions by sequentially enhancing ERM-mediated actin-membrane attachment for force transmission and NM2-dependent contractility.

Publisher

American Association for the Advancement of Science (AAAS)

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