USP33 regulates centrosome biogenesis via deubiquitination of the centriolar protein CP110

Li, Ji; D’Angiolella, Vincenzo; Seeley, E. Scott; Kim, Sehyun; Kobayashi, Tetsuo; Fu, Wenxiang; Campos, Eric I.; Pagano, Michele; Dynlacht, Brian David

doi:10.1038/nature11941

Cited by 124 publications

(127 citation statements)

References 20 publications

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“…However, alternatively, it is possible that centrobin has a direct or indirect role in inhibiting the proteasome, which prevents the degradation of ubiquitinated proteins, CPAP in particular, possibly by affecting the deubiquitinase function. For example, the activity of deubiquitinase USP33 has been linked to the regulation of centriole distal end capping protein, CP110 (60). It is possible that deubiquitination of CPAP, before protease degradation in the proteasome, may be dependent on USP33 or similar enzymes, and high levels of centrobin may have a regulatory effect on them, which needs to be investigated in the future.…”

Section: Discussionmentioning

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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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%

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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“…In addition, another deubiquitinase Usp33 has recently been shown to localize at the centrosome by its binding with CP110 and its activity antagonizes SCF cyclinF ubiquitination of CP110 (ref. 58).…”

Section: Discussionmentioning

confidence: 99%

The deubiquitinating enzyme CYLD controls apical docking of basal bodies in ciliated epithelial cells

et al. 2014

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CYLD is a tumour suppressor gene mutated in familial cylindromatosis, a genetic disorder leading to the development of skin appendage tumours. It encodes a deubiquitinating enzyme that removes Lys63-or linear-linked ubiquitin chains. CYLD was shown to regulate cell proliferation, cell survival and inflammatory responses, through various signalling pathways. Here we show that CYLD localizes at centrosomes and basal bodies via interaction with the centrosomal protein CAP350 and demonstrate that CYLD must be both at the centrosome and catalytically active to promote ciliogenesis independently of NF-kB. In transgenic mice engineered to mimic the smallest truncation found in cylindromatosis patients, CYLD interaction with CAP350 is lost disrupting CYLD centrosome localization, which results in cilia formation defects due to impairment of basal body migration and docking. These results point to an undiscovered regulation of ciliogenesis by Lys63 ubiquitination and provide new perspectives regarding CYLD function that should be considered in the context of cylindromatosis.

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“…Some DUBs have been shown to have important roles in the maintenance of centrosome integrity. USP33 positively regulates centrosome duplication by stabilizing centriolar protein CP110, and USP 33 and CP110 are both upregulated in pancreatic ductal carcinomas 28 in which centrosome amplification is detected. 29 USP44 regulates centrosome positioning to prevent aneuploidy and suppress tumorigenesis.…”

Section: Introductionmentioning

confidence: 99%

A novel role for the deubiquitinase USP1 in the control of centrosome duplication

2016

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Defects in the regulation of centrosome duplication lead to tumorigenesis through abnormal cell division and resulting chromosome missegregation. Therefore, maintenance of accurate centrosome number is critical for cell fate. The deubiquitinating enzyme USP1 plays important roles in DNA repair and cell differentiation. Importantly, increased levels of USP1 are detected in certain types of human cancer, but little is known about the significance of USP1 overexpression in cancer development. Here we show that Usp1 plays a novel role in regulating centrosome duplication. The ectopic expression of wild-type Usp1, but not C90S Usp1 (catalytically inactive mutant form), induced centrosome amplification. Conversely, ablation of Usp1 in mouse embryonic fibroblasts (MEFs) showed a significant delay in centrosome duplication. Moreover, Usp1-induced centrosome amplification caused abnormal mitotic spindles, chromosome missegregation and aneuploidy. Interestingly, loss of inhibitor of DNA binding protein 1 (ID1) suppressed Usp1-induced centrosome amplification. Taken together, our results strongly suggest that Usp1 is involved in the regulation of centrosome duplication, at least in part via ID1, and Usp1 may exert its oncogenic activity, partially through inducing centrosome abnormality.

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USP33 regulates centrosome biogenesis via deubiquitination of the centriolar protein CP110

Cited by 124 publications

References 20 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

The deubiquitinating enzyme CYLD controls apical docking of basal bodies in ciliated epithelial cells

A novel role for the deubiquitinase USP1 in the control of centrosome duplication

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