A putative exchange factor for Rho1 GTPase is required for initiation of cytokinesis in Drosophila

Sergei N. Prokopenko; Anthony Brumby; Louise O’Keefe; Leanne Prior; Yuchun He; Robert Saint; Hugo J. Bellen

A putative exchange factor for Rho1 GTPase is required for initiation of cytokinesis in Drosophila

Program in Developmental Biology, Howard Hughes Medical Institute, and Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, Texas 77030 USA; Department of Genetics, University of Adelaide, Adelaide SA 5005, Australia

Abstract

Cytokinesis ensures the successful completion of the cell cycle and distribution of chromosomes, organelles, and cytoplasm between daughter cells. It is accomplished by formation and constriction of an actomyosin contractile ring that drives the progression of a cleavage furrow. Microinjection experiments and in vitro transfection assays have suggested a requirement for small GTPases of the Rho family in cytokinesis. Yet, the identity of proteins regulating Rho signaling pathways during cytokinesis remains unknown. Here we show that inDrosophila, Pebble (Pbl), a putative exchange factor for Rho GTPases (RhoGEF), is required for the formation of the contractile ring and initiation of cytokinesis. The dynamics of Pbl expression and its distribution during mitosis, as well as structure-function analysis, indicate that it is a key regulatory component of the pathway.pbl interacts genetically with Rho1, but not withRac1 or Cdc42, and Pbl and Rho1 proteins interact in vivo in yeast. Similar to mutations in pbl, loss ofRho1 or expression of a dominant–negative Rho1 blocks cytokinesis. Our results identify Pbl as a RhoGEF specifically required for cytokinesis and linked through Rho1 activity to the reorganization of the actin cytoskeleton at the cleavage furrow.

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