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      A ginseng metabolite, compound K, induces autophagy and apoptosis via generation of reactive oxygen species and activation of JNK in human colon cancer cells

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          Abstract

          Compound K (20-O-( β- D-glucopyranosyl)-20(S)-protopanaxadiol) is an active metabolite of ginsenosides and induces apoptosis in various types of cancer cells. This study investigated the role of autophagy in compound K-induced cell death of human HCT-116 colon cancer cells. Compound K activated an autophagy pathway characterized by the accumulation of vesicles, the increased positive acridine orange-stained cells, the accumulation of LC3-II, and the elevation of autophagic flux. Whereas blockade of compound K-induced autophagy by 3-methyladenein and bafilomycin A1 significantly increased cell viability. In addition, compound K augmented the time-dependent expression of the autophagy-related proteins Atg5, Atg6, and Atg7. However, knockdown of Atg5, Atg6, and Atg7 markedly inhibited the detrimental impact of compound K on LC3-II accumulation and cell vitality. Compound K-provoked autophagy was also linked to the generation of intracellular reactive oxygen species (ROS); both of these processes were mitigated by the pre-treatment of cells with the antioxidant N-acetylcysteine. Moreover, compound K activated the c-Jun NH2-terminal kinase (JNK) signaling pathway, whereas downregulation of JNK by its specific inhibitor SP600125 or by small interfering RNA against JNK attenuated autophagy-mediated cell death in response to compound K. Compound K also provoked apoptosis, as evidenced by an increased number of apoptotic bodies and sub-G 1 hypodiploid cells, enhanced activation of caspase-3 and caspase-9, and modulation of Bcl-2 and Bcl-2-associated X protein expression. Notably, compound K-stimulated autophagy as well as apoptosis was induced by disrupting the interaction between Atg6 and Bcl-2. Taken together, these results indicate that the induction of autophagy and apoptosis by compound K is mediated through ROS generation and JNK activation in human colon cancer cells.

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          The role of Atg proteins in autophagosome formation.

          Noboru Mizushima, Tamotsu Yoshimori, Yoshinori Ohsumi (2011)
          Macroautophagy is mediated by a unique organelle, the autophagosome, which encloses a portion of cytoplasm for delivery to the lysosome. Autophagosome formation is dynamically regulated by starvation and other stresses and involves complicated membrane reorganization. Since the discovery of yeast Atg-related proteins, autophagosome formation has been dissected at the molecular level. In this review we describe the molecular mechanism of autophagosome formation with particular focus on the function of Atg proteins and the long-standing discussion regarding the origin of the autophagosome membrane.
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            Programmed cell death pathways in cancer: a review of apoptosis, autophagy and programmed necrosis.

            L Ouyang, Z. Shi, S. Zhao (2012)
            Programmed cell death (PCD), referring to apoptosis, autophagy and programmed necrosis, is proposed to be death of a cell in any pathological format, when mediated by an intracellular program. These three forms of PCD may jointly decide the fate of cells of malignant neoplasms; apoptosis and programmed necrosis invariably contribute to cell death, whereas autophagy can play either pro-survival or pro-death roles. Recent bulk of accumulating evidence has contributed to a wealth of knowledge facilitating better understanding of cancer initiation and progression with the three distinctive types of cell death. To be able to decipher PCD signalling pathways may aid development of new targeted anti-cancer therapeutic strategies. Thus in this review, we present a brief outline of apoptosis, autophagy and programmed necrosis pathways and apoptosis-related microRNA regulation, in cancer. Taken together, understanding PCD and the complex interplay between apoptosis, autophagy and programmed necrosis may ultimately allow scientists and clinicians to harness the three types of PCD for discovery of further novel drug targets, in the future cancer treatment. © 2012 Blackwell Publishing Ltd.
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              Reactive oxygen species promote TNFalpha-induced death and sustained JNK activation by inhibiting MAP kinase phosphatases.

              Hideaki Kamata, Shi-Ichi Honda, Shin Maeda (2005)
              TNFalpha is a pleiotropic cytokine that induces either cell proliferation or cell death. Inhibition of NF-kappaB activation increases susceptibility to TNFalpha-induced death, concurrent with sustained JNK activation, an important contributor to the death response. Sustained JNK activation in NF-kappaB-deficient cells was suggested to depend on reactive oxygen species (ROS), but how ROS affect JNK activation was unclear. We now show that TNFalpha-induced ROS, whose accumulation is suppressed by mitochondrial superoxide dismutase, cause oxidation and inhibition of JNK-inactivating phosphatases by converting their catalytic cysteine to sulfenic acid. This results in sustained JNK activation, which is required for cytochrome c release and caspase 3 cleavage, as well as necrotic cell death. Treatment of cells or experimental animals with an antioxidant prevents H(2)O(2) accumulation, JNK phosphatase oxidation, sustained JNK activity, and both forms of cell death. Antioxidant treatment also prevents TNFalpha-mediated fulminant liver failure without affecting liver regeneration.
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                Author and article information

                Journal
                Journal ID (nlm-ta): Cell Death Dis
                Journal ID (iso-abbrev): Cell Death Dis
                Title: Cell Death & Disease
                Publisher: Nature Publishing Group
                ISSN (Electronic): 2041-4889
                Publication date (Print): August 2013
                Publication date (Electronic): 01 August 2013
                Publication date PMC-release: 1 August 2013
                Volume: 4
                Issue: 8
                Page: e750
                Affiliations
                [1 ]School of Medicine and Institute for Nuclear Science and Technology, Jeju National University , Jeju, Korea
                [2 ]Department of Neuroscience, College of Medicine, Ewha Womans University , Seoul, Korea
                [3 ]Department of Microbial Chemistry, College of Pharmacy, Kyung Hee University , Seoul, Korea
                [4 ]Department of Biochemistry, College of Oriental Medicine and Research Institute of Oriental Medicine, Dongeui University , Pusan, Korea
                [5 ]Department of Chemistry, Research Institute for Natural Sciences, Hanyang University , Seoul, Korea
                [6 ]Cancer Research Institute, Seoul National University College of Medicine , Seoul, Korea
                Author notes
                [* ]School of Medicine, Jeju National University , Jeju 690-756, Korea. Tel: +82 64 7543838; Fax: +82 64 7022687; E-mail: jinwonh@ 123456jejunu.ac.kr
                Article
                Publisher Item ID: cddis2013273
                DOI: 10.1038/cddis.2013.273
                PMC ID: 3763435
                PubMed ID: 23907464
                SO-VID: 983e0b56-0a52-43f7-9269-9f56a0561277
                Copyright © Copyright © 2013 Macmillan Publishers Limited
                License:

                This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivs 3.0 Unported License. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-nd/3.0/

                History
                Date received : 14 March 2013
                Date revision received : 26 May 2013
                Date accepted : 19 June 2013
                Categories
                Subject: Original Article

                ScienceOpen disciplines: Cell biology
                Keywords: apoptosis,autophagy,compound k,reactive oxygen species,colon cancer
                Data availability:
                ScienceOpen disciplines: Cell biology
                Keywords: apoptosis, autophagy, compound k, reactive oxygen species, colon cancer

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