Determination of substrate specificity and putative substrates of Chk2 kinase |
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| Authors: | Seo Gil-Ju Kim Se-Eun Lee Young-Man Lee Jeong-Won Lee Jae-Rin Hahn Myong-Joon Kim Seong-Tae |
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| Affiliation: | Department of Molecular Cellular Biology, Sungkyunkwan University School of Medicine, Samsung Biomedical Research Institute, 300 Chunchun-Dong, Changan-Ku, 440-746, Suwon, Kyunggi-Do, Republic of Korea. |
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| Abstract: | Chk2/hCds1, the human homolog of Saccharomyces cerevisiae Rad53p and Schizosaccharomyces pombe Cds1p, plays a critical role in the DNA damage checkpoint pathway. While several in vivo targets of Chk2 have been identified, the other target proteins of Chk2 responsible for multiple functions, such as cell cycle arrest, DNA repair, and apoptosis, remain to be elucidated. We utilized the GST-peptide approach to identify physiological substrates for Chk2. Mutational analyses using GST-linked Cdc25A containing serine 123 revealed that residues at positions -5 and -3 are critical determinants for the recognition of the Chk2 substrate. We determined the general phosphorylation consensus sequence and identified in vitro targets of Chk2 using GST peptides as substrates. The newly identified in vitro target proteins include Abl1, Bub1R, Bub1, Bub3, Psk-H1, Smc3, Plk1, Cdc25B, Dcamkl1, Mre11, Pms1, and Xrcc9. |
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| Keywords: | Chk2 Cdc25A GST-peptide method DNA damage response pathway Substrate specificity |
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