CEP120 interacts with CPAP and positively regulates centriole elongation

Lin, Yu-Chuan; Wu, Chi-Chang; Lin, Yu‐Chih; Hsu, Wen-Bin; Tang, Tang K.; Chang, Che-Jung

doi:10.1083/jcb.201212060

Cited by 111 publications

(148 citation statements)

References 22 publications

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“…Although several centriolar proteins such as STIL, SAS-6, CEP120, SPICE1, and CEP135 can interact with CPAP and positively regulate the centriole duplication and elongation process (30,32,45,46), this is the first study that uncovers the mechanism by which CPAP levels are regulated in the cell to restrict the centriole length. Earlier we showed that centrobin binds to CPAP directly, and this interaction is essential for maintaining CPAP levels on centrioles (48).…”

Section: Discussionmentioning

confidence: 99%

“…Interestingly, the elongation phase of centriole duplication, which determines centriole length, is completed by the time cells reach mitosis (44). Although CEP120 and SPICE1 are known to promote centriole elongation and interact with CPAP (45,46), they act downstream of CPAP in the centriole duplication process. Therefore, identifying the upstream targets and underlying signals that govern cellular CPAP levels will shed light on how the centriole length is restricted.…”

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confidence: 99%

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Centrobin-mediated Regulation of the Centrosomal Protein 4.1-associated Protein (CPAP) Level Limits Centriole Length during Elongation Stage

Gudi

Haycraft

Bell

et al. 2015

Journal of Biological Chemistry

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Background:The mechanism by which centriole dimensions are regulated is not understood. Results: The absence of centrobin leads to degradation of centrosomal protein 4.1-associated-protein (CPAP). High centrobin levels cause stabilization of CPAP and abnormal centrioles. Conclusion: Centrobin plays a role in the stability and centriole elongation function of CPAP and limits the centriole length. Significance: Identifying the regulatory mechanisms is crucial for understanding centriole biogenesis.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Centrobin-mediated Regulation of the Centrosomal Protein 4.1-associated Protein (CPAP) Level Limits Centriole Length during Elongation Stage

Gudi

Haycraft

Bell

et al. 2015

Journal of Biological Chemistry

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“…The protein CPAP gets recruited to promote the assembly of microtubules onto the cartwheel (Tang et al , 2011a; Cottee et al , 2013; Sharma et al , 2016), and this step is likely assisted by Cep135 (the human homolog of Chlamydomonas Bld10) (Hirono, 2014). CPAP also cooperates with additional proteins, including CP110, in determining the length of nascent centrioles (Kohlmaier et al , 2009; Schmidt et al , 2009; Tang et al , 2009; Comartin et al , 2013; Lin et al , 2013; Sharma et al , 2016). Finally, centriole maturation is completed by the acquisition of subdistal and distal appendages (Paintrand et al , 1992; Tateishi et al , 2013).…”

Section: Introductionmentioning

confidence: 99%

Quantitative analysis of human centrosome architecture by targeted proteomics and fluorescence imaging

et al. 2016

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Centrioles are essential for the formation of centrosomes and cilia. While numerical and/or structural centrosomes aberrations are implicated in cancer, mutations in centriolar and centrosomal proteins are genetically linked to ciliopathies, microcephaly, and dwarfism. The evolutionarily conserved mechanisms underlying centrosome biogenesis are centered on a set of key proteins, including Plk4, Sas‐6, and STIL, whose exact levels are critical to ensure accurate reproduction of centrioles during cell cycle progression. However, neither the intracellular levels of centrosomal proteins nor their stoichiometry within centrosomes is presently known. Here, we have used two complementary approaches, targeted proteomics and EGFP‐tagging of centrosomal proteins at endogenous loci, to measure protein abundance in cultured human cells and purified centrosomes. Our results provide a first assessment of the absolute and relative amounts of major components of the human centrosome. Specifically, they predict that human centriolar cartwheels comprise up to 16 stacked hubs and 1 molecule of STIL for every dimer of Sas‐6. This type of quantitative information will help guide future studies of the molecular basis of centrosome assembly and function.

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“…Some of the components identified as essential for centriole assembly also contribute to centriolar microtubule elongation. Sas-4/ CPAP, for example, promotes the polymerization of centriolar microtubules in cooperation with CEP120, which localizes preferentially to the daughter centriole Comartin et al 2013;Lin et al 2013b). Overexpression of either CPAP or CEP120 results in excessively long centrioles and their depletion abolishes this phenotype (Comartin et al 2013;Lin et al 2013b).…”

Section: Centriole Elongationmentioning

confidence: 99%

“…Sas-4/ CPAP, for example, promotes the polymerization of centriolar microtubules in cooperation with CEP120, which localizes preferentially to the daughter centriole Comartin et al 2013;Lin et al 2013b). Overexpression of either CPAP or CEP120 results in excessively long centrioles and their depletion abolishes this phenotype (Comartin et al 2013;Lin et al 2013b). CEP120 also interacts with SPICE1 that is required for centriole duplication, spindle formation, and chromosome congression (Archinti et al 2010).…”

Section: Centriole Elongationmentioning

confidence: 99%

The Centrosome and Its Duplication Cycle

Hagan

Glover

2015

Cold Spring Harb Perspect Biol

210

194

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CEP120 interacts with CPAP and positively regulates centriole elongation

Abstract: CEP120 cooperates with CPAP to promote centriole elongation in a cell cycle– and microtubule-dependent manner.

Cited by 111 publications

References 22 publications

Centrobin-mediated Regulation of the Centrosomal Protein 4.1-associated Protein (CPAP) Level Limits Centriole Length during Elongation Stage

Centrobin-mediated Regulation of the Centrosomal Protein 4.1-associated Protein (CPAP) Level Limits Centriole Length during Elongation Stage

Quantitative analysis of human centrosome architecture by targeted proteomics and fluorescence imaging

The Centrosome and Its Duplication Cycle

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