Targeting of Nphp3 to the primary cilia is controlled by an N‐terminal myristoylation site and coiled‐coil domains

Nakata, Kana; Shiba, Dai; Kobayashi, Daigo; Yokoyama, Tetsuji

doi:10.1002/cm.21014

Cited by 35 publications

(44 citation statements)

References 38 publications

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“…Unc119b recognizes the myristoylated amino-terminal residues of both Nphp3 and Cystin, thereby protecting them from interaction with the lipid bilayer (Wright et al 2011). Only when bound to cargo can Unc119b enter the cilium across the TZ, where it encounters Arl3, a small GTP-binding protein that binds to and induces the dissociation of the Unc119-cargo complex, thereby allowing the myristoylated cargo to associate with the ciliary membrane (Wright et al 2011; Zhang et al 2011; Nakata et al 2012). In turn, Arl3 activity is regulated by an Arl3-GAP (RP2) and an Arl3-GEF (Arl13b), which regulate its association with GDP or GTP and, therefore, its activity (Wright et al 2011; Gotthardt et al 2015).…”

Section: Transition Zonementioning

confidence: 99%

Open Sesame: How Transition Fibers and the Transition Zone Control Ciliary Composition

Garcia-Gonzalo

Reiter

2016

Cold Spring Harb Perspect Biol

228

227

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Cilia are plasma membrane protrusions that act as cellular propellers or antennae. To perform these functions, cilia must maintain a composition distinct from those of the contiguous cytosol and plasma membrane. The specialized composition of the cilium depends on the ciliary gate, the region at the ciliary base separating the cilium from the rest of the cell. The ciliary gate’s main structural features are electron dense struts connecting microtubules to the adjacent membrane. These structures include the transition fibers, which connect the distal basal body to the base of the ciliary membrane, and the Y-links, which connect the proximal axoneme and ciliary membrane within the transition zone. Both transition fibers and Y-links form early during ciliogenesis and play key roles in ciliary assembly and trafficking. Accordingly, many human ciliopathies are caused by mutations that perturb ciliary gate function.

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Section: Transition Zonementioning

confidence: 99%

Open Sesame: How Transition Fibers and the Transition Zone Control Ciliary Composition

Garcia-Gonzalo

Reiter

2016

Cold Spring Harb Perspect Biol

228

227

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“…The PC1-CTT contains more than one CTS An N-terminal fragment containing two coiled-coil motifs has been shown to be necessary and sufficient to target Nphp3 to the primary cilia, functioning as a CTS (Nakata et al, 2012). We next tested whether the coiled-coil motif in the PC1-CTT or the PC1-CTT itself is sufficient to target foreign proteins to the cilia.…”

Section: Multiple Sequences In the C-terminus Of Pc1 Contribute To CImentioning

confidence: 99%

Regulation of polycystin-1 ciliary trafficking by motifs at its C-terminus and polycystin-2 but not cleavage at GPS site

Yao

El-Jouni

et al. 2015

Journal of Cell Science

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Failure to localize membrane proteins to the primary cilium causes a group of diseases collectively named ciliopathies. Polycystin-1 (PC1, also known as PKD1) is a large ciliary membrane protein defective in autosomal dominant polycystic kidney disease (ADPKD). Here, we developed a large set of PC1 expression constructs and identified multiple sequences, including a coiled-coil motif in the C-terminal tail of PC1, regulating full-length PC1 trafficking to the primary cilium. Ciliary trafficking of wild-type and mutant PC1 depends on the dose of polycystin-2 (PC2, also known as PKD2), and the formation of a PC1-PC2 complex. Modulation of the ciliary trafficking module mediated by the VxP ciliary-targeting sequence and Arf4 and Asap1 does not affect the ciliary localization of full-length PC1. PC1 also promotes PC2 ciliary trafficking. PC2 mutations truncating its C-terminal tail but not those changing the VxP sequence to AxA or impairing the pore of the channel, leading to a dead channel, affect PC1 ciliary trafficking. Cleavage at the GPCR proteolytic site (GPS) of PC1 is not required for PC1 trafficking to cilia. We propose a mutually dependent model for the ciliary trafficking of PC1 and PC2, and that PC1 ciliary trafficking is regulated by multiple cis-acting elements. As all pathogenic PC1 mutations tested here are defective in ciliary trafficking, ciliary trafficking might serve as a functional read-out for ADPKD.

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Section: Transport Of Cytosolic Proteinsmentioning

confidence: 99%

“…The N-terminal myristoylation motif of NPHP3 is necessary for its ciliary localization 188 . This sequence is, however, insufficient for ciliary targeting, which indicates that additional signals in the NPHP3 polypeptide contribute to ciliary localization 188 . An additional layer of complexity in the ciliary targeting of NPHP3 has been revealed by observations that an N-terminal coiled-coil domain of NPHP3, which does not include the myristoylation site, is both necessary and sufficient for targeting to the ciliary centriole.…”

Section: Transport Of Cytosolic Proteinsmentioning

confidence: 99%

“…In photoreceptor cells, it may also function as a solubilization factor during cytoplasmic transport of the ciliary Transducin 186 . Finally, NPHP3 transport seems to proceed independently from the ciliary pore Ran/Importin system 188 . Thus, lipidated proteins appear to follow their own unique traffic rules during cilia-directed transport.…”

Section: Transport Of Cytosolic Proteinsmentioning

confidence: 99%

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From the cytoplasm into the cilium: Bon voyage

Malicki

Avidor‐Reiss

2014

Organogenesis

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The primary cilium compartmentalizes a tiny fraction of the cell surface and volume, yet many proteins are highly enriched in this area and so efficient mechanisms are necessary to concentrate them in the ciliary compartment. Here we review mechanisms that are thought to deliver protein cargo to the base of cilia and are likely to interact with ciliary gating mechanisms. Given the immense variety of ciliary cytosolic and transmembrane proteins, it is almost certain that multiple, albeit frequently interconnected, pathways mediate this process. It is also clear that none of these pathways is fully understood at the present time. Mechanisms that are discussed below facilitate ciliary localization of structural and signaling molecules, which include receptors, G-proteins, ion channels, and enzymes. These mechanisms form a basis for every aspect of cilia function in early embryonic patterning, organ morphogenesis, sensory perception and elsewhere.

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Targeting of Nphp3 to the primary cilia is controlled by an N‐terminal myristoylation site and coiled‐coil domains

Cited by 35 publications

References 38 publications

Open Sesame: How Transition Fibers and the Transition Zone Control Ciliary Composition

Open Sesame: How Transition Fibers and the Transition Zone Control Ciliary Composition

Regulation of polycystin-1 ciliary trafficking by motifs at its C-terminus and polycystin-2 but not cleavage at GPS site

From the cytoplasm into the cilium: Bon voyage

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