Moniliformediquinone induces in vitro and in vivo antitumor activity through glutathione involved DNA damage response and mitochondrial stress in human hormone refractory prostate cancer
Journal
Journal of Urology
Journal Volume
191
Journal Issue
5
Pages
1429-1438
Date Issued
2014
Author(s)
Abstract
Purpose Hormone refractory metastatic prostate cancer is a major obstacle in clinical treatment. The key focus of this study was the discovery and development of a potential agent for this disease. Materials and Methods Several pharmacological and biochemical assays were used to characterize the apoptotic signaling pathways of moniliformediquinone, a natural product, in hormone refractory metastatic prostate cancer. Results Moniliformediquinone induced cell cycle arrest at the S-phase and subsequent apoptosis in the hormone refractory metastatic prostate cancer cell lines PC-3 and DU-145. Further examination showed that moniliformediquinone induced a DNA damage response associated with Chk1, Chk2, c-Jun and JNK activation. Mitochondrial apoptosis pathways were also activated, including loss of mitochondrial membrane potential, cytochrome c release, and activation of caspase-9 and 3. The antioxidant and glutathione precursor N-acetylcysteine, and the antioxidant Trolox? completely abolished moniliformediquinone induced generation of reactive oxygen species. However, N-acetylcysteine but not Trolox blocked moniliformediquinone mediated apoptosis and related signaling cascades. Further identification showed that moniliformediquinone alone did not conjugate glutathione but significantly decreased cellular glutathione levels. The in vivo study revealed that moniliformediquinone completely inhibited tumor growth with no weight loss. Conclusions Our data suggest that moniliformediquinone is a potential anticancer agent for hormone refractory metastatic prostate cancer by decreasing cellular glutathione, leading to a DNA damage response and cell cycle arrest at the S-phase. Mitochondrial stress also occurs due to moniliformediquinone action through loss of mitochondrial membrane potential and cytochrome c release, which in turn induce the activation of caspase cascades and apoptotic cell death. ? 2014 by American Urological Association Education and Research, Inc.
Subjects
apoptosis; castration-resistant; Dendrobium; glutathione; mitochondria; prostatic neoplasms
SDGs
Other Subjects
acetylcysteine; antineoplastic agent; caspase 3; caspase 9; checkpoint kinase 1; checkpoint kinase 2; cytochrome c; glutathione; moniliformediquinone; protein c jun; reactive oxygen metabolite; stress activated protein kinase; trolox C; unclassified drug; acetylcysteine; antineoplastic agent; caspase 2; caspase 7; caspase 8; DNA A; moniliformediquinone; natural product; paclitaxel; animal cell; animal experiment; animal model; antineoplastic activity; antiproliferative activity; apoptosis; article; cancer cell culture; cancer inhibition; castration resistant prostate cancer; cell cycle S phase; cell proliferation; cell stress; cell synchronization; controlled study; DNA damage; DNA strand breakage; drug cytotoxicity; drug efficacy; G1 phase cell cycle checkpoint; in vitro study; in vivo study; mitochondrial gene; mitochondrial membrane potential; mouse; nonhuman; oxidative stress; priority journal; protein secretion; S phase cell cycle checkpoint; tumor volume; antiproliferative activity; Article; cancer growth; cancer inhibition; cancer size; castration resistant prostate cancer; cell cycle arrest; cell cycle progression; cell level; cellular stress response; cytotoxicity; glutathione metabolism; human; human cell; male; mitochondrial stress; mitochondrion; prostate cancer cell line; signal transduction; weight reduction; apoptosis; castration-resistant; Dendrobium; glutathione; mitochondria; prostatic neoplasms; Antineoplastic Agents; DNA Damage; Drug Screening Assays, Antitumor; Glutathione; Humans; Male; Mitochondria; Phenanthrenes; Prostatic Neoplasms, Castration-Resistant; Quinones; Tumor Cells, Cultured
Type
journal article