Regulation of ciliary retrograde protein trafficking by the Joubert syndrome proteins ARL13B and INPP5E

Nozaki, Shohei; Katoh, Yohei; Terada, Masaya; Michisaka, Saki; Funabashi, Teruki; Takahashi, Shouji; Kontani, Kenji; Nakayama, Kazuhisa

doi:10.1242/jcs.197004

Cited by 73 publications

(106 citation statements)

References 60 publications

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“…Previous studies have shown that Arl13b loss leads to aberrant SMO accumulation in cilia, suggesting that Arl13b limits the ciliary accumulation of SMO, possibly by promoting its ciliary export . We wondered, therefore, whether elevated ciliary ARL13B levels in RAB35‐depleted cells are required for the SMO localisation defect in these cells.…”

Section: Resultsmentioning

confidence: 94%

“…Arl13b consists of an N‐terminal guanine nucleotide‐binding (G) domain and an unusually long C‐terminal tail with coiled coil (CC) and proline‐rich (PR) domains (Fig B) . All these domains were previously shown to be important for protein–protein interactions; for example, IFT‐B proteins interact with Arl13b via its PR domain, while INPP5E binds to the G‐domain . Arl13b also contains a C‐terminal RVEP motif for ciliary targeting and N‐terminal palmitoylation for ciliary membrane anchoring .…”

Section: Resultsmentioning

confidence: 99%

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Rab35 controls cilium length, function and membrane composition

et al. 2019

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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.

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Section: Resultsmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

Rab35 controls cilium length, function and membrane composition

et al. 2019

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“…Expression vectors for the IFT-B subunits were described previously (Katoh et al. , 2016; Nozaki et al. , 2017).…”

Section: Methodsmentioning

confidence: 99%

“…The cell lysates were immunoprecipitated with GST–anti-GFP Nb prebound to glutathione–Sepharose 4B beads, and bound proteins were subjected to SDS–PAGE and immunoblotting analysis using anti-HA, anti-mRFP, anti-tRFP, or anti-GFP antibodies as described previously (Katoh et al. , 2015, 2016; Nozaki et al. , 2017).…”

Section: Methodsmentioning

confidence: 99%

RABL2 interacts with the intraflagellar transport-B complex and CEP19 and participates in ciliary assembly

Nishijima

Hagiya

Kubo

et al. 2017

MBoC

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104

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“…Defects in the IFT components have been shown to cause a spectrum of diseases, ranging from developmental defects to obesity, diabetes, and cancer. Many of these diseases, or ciliopathies, manifest as genetic syndromes, such as Joubert syndrome, Bardet-Biedel (BBS), Meckel-Gruber (MKS), and Nephronophthisis (NPHP)(Barker et al, 2014; Nozaki et al, 2017; Srivastava and Sayer, 2014; Su et al, 2014; Suspitsin and Imyanitov, 2016). …”

Section: Introductionmentioning

confidence: 99%

Intraflagellar transporter protein (IFT27), an IFT25 binding partner, is essential for male fertility and spermiogenesis in mice

Zhang

Liu

et al. 2017

Developmental Biology

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Intraflagellar transport (IFT) is an evolutionarily conserved mechanism essential for the assembly and maintenance of most eukaryotic cilia and flagella. In mice, mutations in IFT proteins have been shown to cause several ciliopathies including retinal degeneration, polycystic kidney disease, and hearing loss. However, little is known about its role in the formation of the sperm tail, which has the longest flagella of mammalian cells. IFT27 is a component of IFT-B complex and binds to IFT25 directly. In mice, IFT27 is highly expressed in the testis. To investigate the role of IFT27 in male germ cells, the floxed Ift27 mice were bred with Stra8-iCre mice so that the Ift27 gene was disrupted in spermatocytes/spermatids. The Ift27:Stra8-iCre mutant mice did not show any gross abnormalities, and all of the mutant mice survive to adulthood. There was no difference between testis weight/body weight between controls and mutant mice. All adult homozygous mutant males examined were completely infertile. Histological examination of the testes revealed abnormally developed germ cells during the spermiogenesis phase. The epididymis contained round bodies of cytoplasm. Sperm number was significantly reduced compared to the controls and only about 2% of them remained significantly reduced motility. Examination of epididymal sperm by light microscopy and SEM revealed multiple morphological abnormalities including round heads, short and bent tails, abnormal thickness of sperm tails in some areas, and swollen tail tips in some sperm. TEM examination of epididymal sperm showed that most sperm lost the “9+2” axoneme structure, and the mitochondria sheath, fibrous sheath, and outer dense fibers were also disorganized. Some sperm flagella also lost cell membrane. Levels of IFT25 and IFT81 were significantly reduced in the testis of the conditional Ift27 knockout mice, and levels of IFT20, IFT74, and IFT140 were not changed. Sperm lipid rafts, which were disrupted in the conditional Ift25 knockout mice, appeared to be normal in the conditional Ift27 knockout mice. Our findings suggest that like IFT25, IFT27, even though not required to ciliogenesis in somatic cells, is essential for sperm flagella formation, sperm function, and male fertility in mice. IFT25 and IFT27 control sperm formation/function through many common mechanisms, but IFT25 has additional roles beyond IFT27.

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Regulation of ciliary retrograde protein trafficking by the Joubert syndrome proteins ARL13B and INPP5E

Cited by 73 publications

References 60 publications

Rab35 controls cilium length, function and membrane composition

Rab35 controls cilium length, function and membrane composition

RABL2 interacts with the intraflagellar transport-B complex and CEP19 and participates in ciliary assembly

Intraflagellar transporter protein (IFT27), an IFT25 binding partner, is essential for male fertility and spermiogenesis in mice

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