a phospho-proteomic screen identifies substrates of the checkpoint kinase chk1phospho-proteomic屏幕识别检查点激酶chk1的基质.pdfVIP
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a phospho-proteomic screen identifies substrates of the checkpoint kinase chk1phospho-proteomic屏幕识别检查点激酶chk1的基质
Blasius et al. Genome Biology 2011, 12:R78
/content/12/8/R78
RESEARCH Open Access
A phospho-proteomic screen identifies substrates
of the checkpoint kinase Chk1
1† 1† 1 2 2
Melanie Blasius , Josep V Forment , Neha Thakkar , Sebastian A Wagner , Chunaram Choudhary and
Stephen P Jackson1*
Abstract
Background: The cell-cycle checkpoint kinase Chk1 is essential in mammalian cells due to its roles in controlling
processes such as DNA replication, mitosis and DNA-damage responses. Despite its paramount importance, how
Chk1 controls these functions remains unclear, mainly because very few Chk1 substrates have hitherto been
identified.
Results: Here, we combine a chemical genetics approach with high-resolution mass spectrometry to identify novel
Chk1 substrates and their phosphorylation sites. The list of targets produced reveals the potential impact of Chk1
function not only on processes where Chk1 was already known to be involved, but also on other key cellular
events such as transcription, RNA splicing and cell fate determination. In addition, we validate and explore the
phosphorylation of transcriptional co-repressor KAP1 Ser473 as a novel DNA-damage-induced Chk1 site.
Conclusions: By providing a substantial set of potential Chk1 substrates, we present opportunities for studying
unanticipated functions for Chk1 in controlling a wide range of cellular processes. We also refine the Chk1
consensus sequence, facilitating the future prediction of Chk1 target sites. In addition, our identification of KAP1
Ser473 phosphorylation as a robust readout for Chk1 activity could be used to explore the in vivo effects of Chk1
inhibitors that are being developed for clinical eva
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