: Bardet-Biedl syndrome (BBS) is a ciliopathy characterized by retinal degeneration, obesity, renal abnormalities, postaxial polydactyly, and developmental defects. Genes mutated in BBS encode for components and regulators of the BBSome, an octameric complex that controls the trafficking of cargos and receptors within the primary cilium. Although both structure and function of the BBSome have been extensively studied, the impact of ubiquitin signaling on BBSome is largely unknown. We identify the E3 ubiquitin ligase PJA2 as a novel resident of the ciliary compartment and regulator of the BBSome. Upon GPCR-cAMP stimulation, PJA2 ubiquitylates BBSome subunits. We demonstrate that ubiquitylation of BBS1 at lysine 143 increases the stability of the BBSome and promotes its binding to BBS3, an Arf-like GTPase protein controlling the targeting of the BBSome to the ciliary membrane. Downregulation of PJA2 or expression of a ubiquitylation-defective BBS1 mutant (BBS1K143R ) affects the trafficking of G-protein-coupled receptors (GPCRs) and Shh-dependent gene transcription. Expression of BBS1K143R in vivo impairs cilium formation, embryonic development, and photoreceptors' morphogenesis, thus recapitulating the BBS phenotype in the medaka fish model.

Ubiquitylation of BBSome is required for ciliary assembly and signaling / Chiuso, Francesco; Delle Donne, Rossella; Giamundo, Giuliana; Rinaldi, Laura; Borzacchiello, Domenica; Moraca, Federica; Intartaglia, Daniela; Iannucci, Rosa; Senatore, Emanuela; Lignitto, Luca; Garbi, Corrado; Conflitti, Paolo; Catalanotti, Bruno; Conte, Ivan; Feliciello, Antonio. - In: EMBO REPORTS. - ISSN 1469-3178. - (2023). [10.15252/embr.202255571]

Ubiquitylation of BBSome is required for ciliary assembly and signaling

Chiuso, Francesco;Delle Donne, Rossella;Giamundo, Giuliana;Rinaldi, Laura;Borzacchiello, Domenica;Moraca, Federica;Iannucci, Rosa;Senatore, Emanuela;Lignitto, Luca;Garbi, Corrado;Catalanotti, Bruno;Conte, Ivan;Feliciello, Antonio
2023

Abstract

: Bardet-Biedl syndrome (BBS) is a ciliopathy characterized by retinal degeneration, obesity, renal abnormalities, postaxial polydactyly, and developmental defects. Genes mutated in BBS encode for components and regulators of the BBSome, an octameric complex that controls the trafficking of cargos and receptors within the primary cilium. Although both structure and function of the BBSome have been extensively studied, the impact of ubiquitin signaling on BBSome is largely unknown. We identify the E3 ubiquitin ligase PJA2 as a novel resident of the ciliary compartment and regulator of the BBSome. Upon GPCR-cAMP stimulation, PJA2 ubiquitylates BBSome subunits. We demonstrate that ubiquitylation of BBS1 at lysine 143 increases the stability of the BBSome and promotes its binding to BBS3, an Arf-like GTPase protein controlling the targeting of the BBSome to the ciliary membrane. Downregulation of PJA2 or expression of a ubiquitylation-defective BBS1 mutant (BBS1K143R ) affects the trafficking of G-protein-coupled receptors (GPCRs) and Shh-dependent gene transcription. Expression of BBS1K143R in vivo impairs cilium formation, embryonic development, and photoreceptors' morphogenesis, thus recapitulating the BBS phenotype in the medaka fish model.
2023
Ubiquitylation of BBSome is required for ciliary assembly and signaling / Chiuso, Francesco; Delle Donne, Rossella; Giamundo, Giuliana; Rinaldi, Laura; Borzacchiello, Domenica; Moraca, Federica; Intartaglia, Daniela; Iannucci, Rosa; Senatore, Emanuela; Lignitto, Luca; Garbi, Corrado; Conflitti, Paolo; Catalanotti, Bruno; Conte, Ivan; Feliciello, Antonio. - In: EMBO REPORTS. - ISSN 1469-3178. - (2023). [10.15252/embr.202255571]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11588/913579
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