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Local temporal Rac1-GTP nadirs and peaks restrict cell protrusions and retractions.

Jianjiang HuXiaowei GongStaffan Strömblad
Published in: Science advances (2022)
Cells probe their microenvironment using membrane protrusion-retraction cycles. Spatiotemporal coordination of Rac1 and RhoA GTP-binding activities initiates and reinforces protrusions and retractions, but the control of their finite lifetime remains unclear. We examined the relations of Rac1 and RhoA GTP-binding levels to key protrusion and retraction events, as well as to cell-ECM traction forces at physiologically relevant ECM stiffness. High RhoA-GTP preceded retractions and Rac1-GTP elevation before protrusions. Notable temporal Rac1-GTP nadirs and peaks occurred at the maximal edge velocity of local membrane protrusions and retractions, respectively, followed by declined edge velocity. Moreover, altered local Rac1-GTP consistently preceded similarly altered traction force. Local optogenetic Rac1-GTP perturbations defined a function of Rac1 in restricting protrusions and retractions and in promoting local traction force. Together, we show that Rac1 plays a fundamental role in restricting the size and durability of protrusions and retractions, plausibly in part through controlling traction forces.
Keyphrases
  • cell migration
  • single cell
  • stem cells
  • cell therapy
  • induced apoptosis
  • signaling pathway
  • cell death
  • body composition
  • extracellular matrix
  • blood flow
  • high intensity
  • cell cycle arrest