| Literature DB >> 31432619 |
Stefanie Kuhns1,2, Cecília Seixas3, Sara Pestana3, Bárbara Tavares3, Renata Nogueira3, Raquel Jacinto3, José S Ramalho3, Jeremy C Simpson4, Jens S Andersen2, Arnaud Echard5, Susana S Lopes3, Duarte C Barral3, Oliver E Blacque1.
Abstract
Rab and Arl guanine nucleotide-binding (G) proteins regulate trafficking pathways essential for the formation, function and composition of primary cilia, which are sensory devices associated with Sonic hedgehog (Shh) signalling and ciliopathies. Here, using mammalian cells and zebrafish, we uncover ciliary functions for Rab35, a multitasking G protein with endocytic recycling, actin remodelling and cytokinesis roles. Rab35 loss via siRNAs, morpholinos or knockout reduces cilium length in mammalian cells and the zebrafish left-right organiser (Kupffer's vesicle) and causes motile cilia-associated left-right asymmetry defects. Consistent with these observations, GFP-Rab35 localises to cilia, as do GEF (DENND1B) and GAP (TBC1D10A) Rab35 regulators, which also regulate ciliary length and Rab35 ciliary localisation. Mammalian Rab35 also controls the ciliary membrane levels of Shh signalling regulators, promoting ciliary targeting of Smoothened, limiting ciliary accumulation of Arl13b and the inositol polyphosphate 5-phosphatase (INPP5E). Rab35 additionally regulates ciliary PI(4,5)P2 levels and interacts with Arl13b. Together, our findings demonstrate roles for Rab35 in regulating cilium length, function and membrane composition and implicate Rab35 in pathways controlling the ciliary levels of Shh signal regulators.Entities:
Keywords: Arl13b; Rab35; Smoothened; cilia; left-right asymmetry
Mesh:
Substances:
Year: 2019 PMID: 31432619 PMCID: PMC6776896 DOI: 10.15252/embr.201847625
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807