Ezrin, radixin, and moesin are dispensable for macrophage migration and cellular cortex mechanics

Author:

Verdys PerrineORCID,Rey Barroso JavierORCID,Girel Adeline,Vermeil Joseph,Bergert MartinORCID,Sanchez ThibautORCID,Métais Arnaud,Mangeat Thomas,Bellard Elisabeth,Bigot Claire,Astarie-Dequeker Catherine,Labrousse ArnaudORCID,Girard Jean-Philippe,Maridonneau-Parini Isabelle,Vérollet ChristelORCID,Lagarrigue Frédéric,Diz-Muñoz AlbaORCID,Heuvingh JulienORCID,Piel Matthieu,du Roure OliviaORCID,Le Cabec VéroniqueORCID,Carréno SébastienORCID,Poincloux RenaudORCID

Abstract

AbstractThe cellular cortex provides crucial mechanical support and plays critical roles during cell division and migration. The proteins of the ERM family, comprised of ezrin, radixin, and moesin, are central to these processes by linking the plasma membrane to the actin cytoskeleton. To investigate the contributions of the ERM proteins to leukocyte migration, we generated single and triple ERM knockout macrophages. Surprisingly, we found that even in the absence of ERM proteins, macrophages still form the different actin structures promoting cell migration, such as filopodia, lamellipodia, podosomes, and ruffles. Furthermore, we discovered that, unlike every other cell type previously investigated, the single or triple knockout of ERM proteins does not affect macrophage migration in diverse contexts. Finally, we demonstrated that the loss of ERMs in macrophages does not affect the mechanical properties of their cortex. These findings challenge the notion that ERMs are universally essential for cortex mechanics and cell migration and support the notion that the macrophage cortex may have diverged from that of other cells to allow for their uniquely adaptive cortical plasticity.

Funder

Universite Toulouse III Paul Sabatier UT3

ITMO Cancer

CIHR

Globalink MITACS

ANR

IPGG

EMBL

Ligue Nationale Contre le Cancer

Publisher

Springer Science and Business Media LLC

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