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p53 regulates oxidative stress-mediated retrograde signaling: A novel mechanism for chemotherapy-induced cardiac injury

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dc.contributor.authorJoyce M. Velezen_US
dc.contributor.authorSumitra Miriyalaen_US
dc.contributor.authorRamaneeya Nithipongvanitchen_US
dc.contributor.authorTeresa Noelen_US
dc.contributor.authorChotiros D. Plabpluengen_US
dc.contributor.authorTerry Oberleyen_US
dc.contributor.authorPaiboon Jungsuwadeeen_US
dc.contributor.authorHolly van Remmenen_US
dc.contributor.authorMary Voreen_US
dc.contributor.authorDaret K. St Clairen_US
dc.contributor.otherUniversity of Kentucky College of Medicineen_US
dc.contributor.otherUniversity of Wisconsin Madisonen_US
dc.contributor.otherVA Medical Centeren_US
dc.contributor.otherMahidol Universityen_US
dc.contributor.otherUniversity of Texas Health Science Center at San Antonioen_US
dc.date.accessioned2018-05-03T07:56:51Z
dc.date.available2018-05-03T07:56:51Z
dc.date.issued2011-04-07en_US
dc.description.abstractThe side effects of cancer therapy on normal tissues limit the success of therapy. Generation of reactive oxygen species (ROS) has been implicated for numerous chemotherapeutic agents including doxorubicin (DOX), a potent cancer chemotherape utic drug. The production of ROS by DOX has been linked to DNA damage, nuclear translocation of p53, and mitochondrial injury; however, the causal relationship and molecular mechanisms underlying these events are unknown. The present study used wild-type (WT) and p53 homozygous knock-out (p53 -/- ) mice to investigate the role of p53 in the crosstalk between mitochondria and nucleus. Injecting mice with DOX (20 mg/kg) causes oxidative stress in cardiac tissue as demonstrated by immunogold analysis of the levels of 4-hydroxy-2′-nonenal (4HNE)-adducted protein, a lipid peroxidation product bound to proteins. 4HNE levels increased in both nuclei and mitochondria of WT DOX-treated mice but only in nuclei of DOX-treated p53 (-/-) mice, implicating a critical role for p53 in causing DOX-induced oxidative stress in mitochondria. The stress-activated protein c-Jun amino-terminal kinase (JNKs) was activated in response to increased 4HNE in WT mice but not p53 (-/-) mice receiving DOX treatment, as determined by co-immunoprecipitation of HNE and pJNK. The activation of JNK in DOX treated WT mice was accompanied by Bcl-2 dissociation from Beclin in mitochondria and induction of type II cell death (autophagic cell death), as evidenced by an increase in LC3-I/LC-3-II ratio and γ-H2AX, a biomarker for DNA damage. The absence of p53 significantly reduces mitochondrial injury, assessed by quantitative morphology, and decline in cardiac function, assessed by left ventricular ejection fraction and fraction shortening. These results demonstrate that p53 plays a critical role in DOX-induced cardiac toxicity, in part, by the induction of oxidative stress mediated retrograde signaling. © 2011 Velez et al.en_US
dc.identifier.citationPLoS ONE. Vol.6, No.3 (2011)en_US
dc.identifier.doi10.1371/journal.pone.0018005en_US
dc.identifier.issn19326203en_US
dc.identifier.other2-s2.0-79953299345en_US
dc.identifier.urihttps://repository.li.mahidol.ac.th/handle/20.500.14594/11330
dc.rightsMahidol Universityen_US
dc.rights.holderSCOPUSen_US
dc.source.urihttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=79953299345&origin=inwarden_US
dc.subjectAgricultural and Biological Sciencesen_US
dc.subjectBiochemistry, Genetics and Molecular Biologyen_US
dc.titlep53 regulates oxidative stress-mediated retrograde signaling: A novel mechanism for chemotherapy-induced cardiac injuryen_US
dc.typeArticleen_US
dspace.entity.typePublication
mu.datasource.scopushttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=79953299345&origin=inwarden_US

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