A class I PI3K signalling network regulates primary cilia disassembly in normal physiology and disease.
Sarah E ConduitWayne PearceAmandeep BhamraBenoit BilangesLaura Bozal-BasterraLazaros C FoukasMathias CobbautSandra D CastilloMohammad Amin DaneshMahreen AdilArkaitz CarracedoMariona GrauperaNeil Q McDonaldPeter J ParkerPedro Rodriguez CutillasSilvia SurinovaBart VanhaesebroeckPublished in: Nature communications (2024)
Primary cilia are antenna-like organelles which sense extracellular cues and act as signalling hubs. Cilia dysfunction causes a heterogeneous group of disorders known as ciliopathy syndromes affecting most organs. Cilia disassembly, the process by which cells lose their cilium, is poorly understood but frequently observed in disease and upon cell transformation. Here, we uncover a role for the PI3Kα signalling enzyme in cilia disassembly. Genetic PI3Kα-hyperactivation, as observed in PIK3CA-related overgrowth spectrum (PROS) and cancer, induced a ciliopathy-like phenotype during mouse development. Mechanistically, PI3Kα and PI3Kβ produce the PIP 3 lipid at the cilia transition zone upon disassembly stimulation. PI3Kα activation initiates cilia disassembly through a kinase signalling axis via the PDK1/PKCι kinases, the CEP170 centrosomal protein and the KIF2A microtubule-depolymerising kinesin. Our data suggest diseases caused by PI3Kα-activation may be considered 'Disorders with Ciliary Contributions', a recently-defined subset of ciliopathies in which some, but not all, of the clinical manifestations result from cilia dysfunction.