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USP29 controls the stability of checkpoint adaptor Claspin by deubiquitination.

Oncogene.. 2014-03; 
MartÍn Y, Cabrera E, Amoedo H, HernÁndez-PÉrez S, DomÍnguez-Kelly R, Freire R. Unidad de InvestigaciÓn, Hospital Universitario de Canarias, Instituto de TecnologÍas BiomÉdicas, La Laguna, Tenerife, Spain.
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摘要

The DNA damage checkpoint is essential for the maintenance of genome integrity after genotoxic stress, and also for cell survival in eukaryotes. Claspin has a key role in the ATR (ATM and Rad3-related)-Chk1 branch of the DNA damage checkpoint and is also required for correct DNA replication. To achieve properly these functions, Claspin is tightly regulated by ubiquitinin-dependent proteasomal degradation, which controls Claspin levels in a DNA-damage- and cell-cycle-dependent manner. Here, we identified a new regulator of Claspin, the ubiquitin-specific peptidase 29, USP29. Downregulation of USP29 destabilizes Claspin, whereas its overexpression promotes an increase in Claspin levels. USP29 interacts with Clasp... More

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