4.8 Article

Selective Chemical Crosslinking Reveals a Cep57-Cep63-Cep152 Centrosomal Complex

Journal

CURRENT BIOLOGY
Volume 23, Issue 3, Pages 265-270

Publisher

CELL PRESS
DOI: 10.1016/j.cub.2012.12.030

Keywords

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Funding

  1. FEBS long-term fellowship
  2. National Centre of Competence in Research in Chemical Biology
  3. Swiss National Science Foundation
  4. Swiss National Science Foundation [CRSII3]
  5. EPFL

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The centrosome functions as the main microtubule-organizing center of animal cells and is crucial for several fundamental cellular processes [1]. Abnormalities in centrosome number and composition correlate with tumor progression [2, 3] and other diseases [4-6]. Although proteomic studies have identified many centrosomal proteins, their interactions are Incompletely characterized [7, 8]. The lack of information on the precise localization and interaction partners for many centrosomal proteins precludes comprehensive understanding of centrosome biology. Here, we utilize a combination of selective chemical crosslinking and superresolution microscopy to reveal novel functional interactions among a set of 31 centrosomal proteins. We reveal that Cep57, Cep63, and Cep152 are parts of a ring-like complex localizing around the proximal end of centrioles. Furthermore, we identify that STIL, together with HsSAS-6, resides at the proximal end of the procentriole, where the cartwheel is located. Our studies also reveal that the known interactors Cep152 and PIk4 reside In two separable structures, suggesting that the kinase PIk4 contacts its substrate Cep152 only transiently, at the centrosome or within the cytoplasm. Our findings provide novel insights Into protein interactions critical for centrosome biology and establish a toolbox for future studies of centrosomal proteins.

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