TY - JOUR T1 - The Role of the Wnt/PCP Formin Daam1 in Renal Ciliogenesis JF - bioRxiv DO - 10.1101/512533 SP - 512533 AU - Mark E. Corkins AU - Vanja Krneta-Stankic AU - Malgorzata Kloc AU - Pierre D. McCrea AU - Andrew B. Gladden AU - Rachel K. Miller Y1 - 2019/01/01 UR - http://biorxiv.org/content/early/2019/01/04/512533.abstract N2 - Kidneys are composed of numerous ciliated epithelial tubules called nephrons. Each nephron functions to reabsorb nutrients and concentrate waste products into urine. Defects in primary cilia are associated with abnormal formation of nephrons and cyst formation in a wide range of kidney disorders. Previous work in Xenopus laevis and zebrafish embryos established that loss of components that make up the Wnt/PCP pathway, Daam1 and ArhGEF19 (wGEF) perturb kidney tubulogenesis. Dishevelled, which activates both the canonical and non-canonical Wnt/PCP pathway, affect cilia formation in multiciliated cells. In this study, we investigated the role of the noncanoncial Wnt/PCP components Daam1 and ArhGEF19 (wGEF) in renal ciliogenesis utilizing polarized mammalian kidney epithelia cells (MDCKII and IMCD3) and Xenopus laevis embryonic kidney. We demonstrate that knockdown of Daam1 and ArhGEF19 in MDCKII and IMCD3 cells leads to loss of cilia, and Daam1’s effect on ciliogenesis is mediated by the formin-activity of Daam1. Moreover, Daam1 co-localizes with the ciliary transport protein IFT88. Interestingly, knocking down Daam1 in Xenopus kidney does not lead to loss of cilia. This data suggests a new role for Daam1 in the formation of primary cilia. ER -