4.7 Article

Cys-141 glutathionylation of human p53: Studies using specific polyclonal antibodies in cancer samples and cell lines

期刊

FREE RADICAL BIOLOGY AND MEDICINE
卷 49, 期 5, 页码 908-917

出版社

ELSEVIER SCIENCE INC
DOI: 10.1016/j.freeradbiomed.2010.06.020

关键词

Oxidative stress; Protein glutathionylation; p53; Posttranslational modification; Cancer biomarker; Reactive cysteines; Signaling; Free radicals

资金

  1. National Institutes of Health [RO1 CA097343, RO3 CA125872]
  2. Laura W Bush Institute for Women's Health, Penman Basin, Texas

向作者/读者索取更多资源

Previously, we reported that human p53 is functionally inactivated by S-glutathionylation at Cys-141 during oxidative and DNA-damaging treatments Here, we describe the presence of thiolated p53 and the dynamic nature of this modification in human tissues using unique and specific polyclonal antibodies raised against a 12-residue p53 peptide bearing a mixed disulfide at Cys-141 The affinity-purified antibodies (glut-p53) were sequence-specific in that they recognized the antigenic peptide but not the unthiolated peptide or a scrambled glutathionylated peptide in ELISAs On immunoblots, the purified antibodies did not react with native p53 or recombinant p53 (rp53), but readily detected the glutathionylated or cysteinylated or ethanethiol-treated rp53 only under nonreducing conditions Untreated HCT116 cells showed low levels of glut-p53. which increased markedly after H2O2. diamide, cisplatin, and doxorubicin treatments Glut-p53 levels decreased sharply after cells were passed into oxidant-free medium. suggesting efficient dethiolation The mutant p53 present in HT29 and T47D human cancer cells was also recognized In vitro, the glut-p53 was rapidly degraded by rabbit reticulocyte lysates Human prostate and prostate cancer tissues showed an abundant presence of glut-p53 in lumina] epithelium, a site well known to generate ROS Melanoma and colon cancer samples were also positive for glut-p53 The availability of the thiolation-specific antibodies should enhance our knowledge of p53 regulation in redox-perturbed states found in various diseases including cancer (C) 2010 Elsevier Inc All rights reserved

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