Literature DB >> 29348145

FBXL13 directs the proteolysis of CEP192 to regulate centrosome homeostasis and cell migration.

Ella Fung1, Carmen Richter2,3, Hong-Bin Yang1, Isabell Schäffer2,3, Roman Fischer4, Benedikt M Kessler4, Florian Bassermann5,3, Vincenzo D'Angiolella6.   

Abstract

Aberrant centrosome organisation with ensuing alterations of microtubule nucleation capacity enables tumour cells to proliferate and invade despite increased genomic instability. CEP192 is a key factor in the initiation process of centrosome duplication and in the control of centrosome microtubule nucleation. However, regulatory means of CEP192 have remained unknown. Here, we report that FBXL13, a binding determinant of SCF (SKP1-CUL1-F-box)-family E3 ubiquitin ligases, is enriched at centrosomes and interacts with the centrosomal proteins Centrin-2, Centrin-3, CEP152 and CEP192. Among these, CEP192 is specifically targeted for proteasomal degradation by FBXL13. Accordingly, induced FBXL13 expression downregulates centrosomal γ-tubulin and disrupts centrosomal microtubule arrays. In addition, depletion of FBXL13 induces high levels of CEP192 and γ-tubulin at the centrosomes with the consequence of defects in cell motility. Together, we characterise FBXL13 as a novel regulator of microtubule nucleation activity and highlight a role in promoting cell motility with potential tumour-promoting implications.
© 2018 The Authors.

Entities:  

Keywords:  CEP192; FBXL13; F‐box protein; centrosome; ubiquitin

Mesh:

Substances:

Year:  2018        PMID: 29348145      PMCID: PMC5836097          DOI: 10.15252/embr.201744799

Source DB:  PubMed          Journal:  EMBO Rep        ISSN: 1469-221X            Impact factor:   8.807


  37 in total

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