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XB-ART-39042
Nat Cell Biol 2009 Mar 01;113:278-85. doi: 10.1038/ncb1835.
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An ATM- and ATR-dependent checkpoint inactivates spindle assembly by targeting CEP63.

Smith E , Dejsuphong D , Balestrini A , Hampel M , Lenz C , Takeda S , Vindigni A , Costanzo V .


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Activation of the protein kinases ATM and ATR following chromosomal breakage prevents initiation of DNA replication and entry into mitosis. However, the effects of ATM and ATR activation in cells already progressing through mitosis are poorly understood. Here we report that ATM and ATR activation induced by DNA double-strand breaks (DSBs) inhibits centrosome-driven spindle assembly in Xenopus laevis mitotic egg extract and somatic cells, delaying mitotic progression. Using a cDNA expression library to screen for ATM and ATR substrates, we identified centrosomal protein CEP63 as an ATM and ATR target required for normal spindle assembly. ATM and ATR phosphorylate Xenopus CEP63 (XCEP63) on Ser 560 and promote its delocalization from the centrosome. Suppression of ATM and ATR activity or mutation of XCEP63 Ser 560 to Ala prevented spindle assembly defects. Consistently, inactivation of the CEP63 gene in avian DT40 cells impaired spindle assembly and prevented ATM- and ATR-dependent effects on mitosis. These data indicate that ATM and ATR control mitotic events in vertebrate cells by targeting CEP63 and centrosome dependent spindle assembly.

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Species referenced: Xenopus laevis
Genes referenced: antxr1 atm atr cep63

References [+] :
Andersen, Proteomic characterization of the human centrosome by protein correlation profiling. 2003, Pubmed