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Concurrent genetic alterations in DNA polymerase proofreading and mismatch repair in human colorectal cancer
Authors:Yoshida Rintaro  Miyashita Kaname  Inoue Mayuko  Shimamoto Akiyoshi  Yan Zhao  Egashira Akinori  Oki Eiji  Kakeji Yoshishiro  Oda Shinya  Maehara Yoshihiko
Affiliation:1Department of Surgery and Science, Graduate School of Medical Sciences, Kyushu University, Fukuoka, Japan;2Department of Hematology, National Kyushu Cancer Center, Fukuoka, Japan;3Cancer Genetics Laboratory, Institute for Clinical Research, National Kyushu Cancer Center, Fukuoka, Japan;4The Third Surgery Department, Liaoning Cancer Hospital and Institute, Shenyang, The People''s Republic of China
Abstract:Genomic sequences encoding the 3' exonuclease (proofreading) domains of both replicative DNA polymerases, pol delta and pol epsilon, were explored simultaneously in human colorectal carcinomas including six established cell lines. Three unequivocal sequence alterations, including one previously reported, were found, and all these were considered as dysfunctional mutations in light of the local amino-acid sequences. In particular, the F367S mutation found in the POLE gene encoding the pol epsilon catalytic subunit, which includes the proofreading domain, is the first found in human diseases. Surprisingly, the tumours carrying these proofreading domain mutations were all defective in DNA mismatch repair (MMR). In addition to the two cell lines with acknowledged MMR gene mutations, the third tumour was also demonstrated to harbour a distinct mutation in MLH1, and indeed exhibited a microsatellite-unstable phenotype. These findings suggest that, in concert with MMR deficiency, defective polymerase proofreading may also contribute to the mutator phenotype observed in human colorectal cancer. Our observations may suggest previously unrecognised complexities in the molecular abnormalities underlying the mutator phenotype in human neoplasms.
Keywords:polymerase delta   polymerase epsilon   proofreading domain   colorectal cancer
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