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Merck

Rac1 promotes kidney collecting duct repair by mechanically coupling cell morphology to mitotic entry.

Science advances (2024-02-07)
Fabian Bock, Xinyu Dong, Shensen Li, Olga M Viquez, Eric Sha, Matthew Tantengco, Elizabeth M Hennen, Erin Plosa, Alireza Ramezani, Kyle L Brown, Young Mi Whang, Andrew S Terker, Juan Pablo Arroyo, David G Harrison, Agnes Fogo, Cord H Brakebusch, Ambra Pozzi, Roy Zent
RESUMEN

Prolonged obstruction of the ureter, which leads to injury of the kidney collecting ducts, results in permanent structural damage, while early reversal allows for repair. Cell structure is defined by the actin cytoskeleton, which is dynamically organized by small Rho guanosine triphosphatases (GTPases). In this study, we identified the Rho GTPase, Rac1, as a driver of postobstructive kidney collecting duct repair. After the relief of ureteric obstruction, Rac1 promoted actin cytoskeletal reconstitution, which was required to maintain normal mitotic morphology allowing for successful cell division. Mechanistically, Rac1 restricted excessive actomyosin activity that stabilized the negative mitotic entry kinase Wee1. This mechanism ensured mechanical G2-M checkpoint stability and prevented premature mitotic entry. The repair defects following injury could be rescued by direct myosin inhibition. Thus, Rac1-dependent control of the actin cytoskeleton integrates with the cell cycle to mediate kidney tubular repair by preventing dysmorphic cells from entering cell division.

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Sigma-Aldrich
(−)-Blebbistatin, solid, synthetic
Sigma-Aldrich
(-)-Blebbistatin, The active enantiomer of (±)-Blebbistatin that accounts for the inhibitory activity towards ATPase and myosin II-dependent cellular processes.
Sigma-Aldrich
Anti-Rac1 Antibody, clone 23A8, clone 23A8, Upstate®, from mouse