Molecular dissection of the centrosome overduplication pathway in S-phase-arrested cells.

Molecular and Cellular Biology
Suzanna L ProsserAndrew M Fry

Abstract

Cancer cells frequently exhibit overduplicated centrosomes that lead to formation of multipolar spindles, chromosome missegregation, and aneuploidy. However, the molecular events involved in centrosome overduplication remain largely unknown. Experimentally, centrosome overduplication is observed in p53-deficient cells arrested in S phase with hydroxyurea. Using this assay, we have identified distinct roles for Cdk2, microtubules, dynein, and Hsp90 in the overduplication of functional centrosomes in mammalian cells and show that Cdk2 is also required for the generation of centriolar satellites. Moreover, we demonstrate that nuclear export is required for centriolar satellite formation and centrosome overduplication, with export inhibitors causing a Cdk-dependent accumulation of nuclear centrin granules. Hence, we propose that centrosome precursors may arise in the nucleus, providing a novel mechanistic explanation for how nuclear Cdk2 can promote centrosome overduplication in the cytoplasm. Furthermore, this study defines a molecular pathway that may be targeted to prevent centrosome overduplication in S-phase-arrested cancer cells.

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Citations

Aug 26, 2010·Journal of Cell Science·Shirin BahmanyarAngela I M Barth
Sep 8, 2012·Journal of Cell Science·Suzanna L ProsserAndrew M Fry
Mar 31, 2012·Cellular and Molecular Life Sciences : CMLS·Tiago J DantasCiaran G Morrison
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Aug 4, 2016·Cellular and Molecular Life Sciences : CMLS·Akiko Hori, Takashi Toda
Nov 26, 2016·Development, Growth & Differentiation·Cheng CuiXuewei Zhang
Nov 5, 2015·Scientific Reports·Satomi MukaiHiroshi Nojima
Jun 23, 2018·Cells·Julie C NielsenSimon Bekker-Jensen
Aug 27, 2009·Journal of Cell Science·Ulf R Klein, Erich A Nigg
Jul 17, 2012·Journal of Cell Science·Christopher J StaplesSpencer J Collis

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