Transgenic mitochondrial superoxide dismutase and mitochondrially targeted catalase prevent antiretroviral-induced oxidative stress and cardiomyopathy

Kohler, James J.; Cucoranu, Ioan; Fields, Earl; Green, Elgin; He, Stanley; Hoying, Amy; Russ, Rodney; Abuin, Allison; Johnson, David M.; Hosseini, Seyed Hamzeh; Raper, C Michael; Lewis, William

doi:10.1038/labinvest.2009.39

Cited by 53 publications

(43 citation statements)

References 55 publications

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“…AZT causes cardiac gene expression changes, altered DNA methylation, and changed SAM abundance. These results support and correlate mechanistically with pathophysiological changes of CM that we reported previously (20). In those studies, AZT caused CM to develop in wild-type mice (WT), while MCAT was able to prevent that CM.…”

supporting

confidence: 91%

“…Our previous work identified oxidative stress to be a critical component in the development of CM in AZT-treated mice (20). In those studies, pathophysiological changes in cardiac mass and structure were identified following 35 days of AZT treatment, and these changes could be attenuated or prevented by enhanced ROS scavenging by MCAT (7)(8)(9).…”

Section: Discussionmentioning

confidence: 97%

“…After 35 days, mice underwent cardiac physiological, histological, and molecular analyses according to our previously published protocols (20). All biomolecular analyses used left ventricle (LV) tissue sections.…”

Section: Methodsmentioning

confidence: 99%

“…(27). We showed that mitochondrial dysfunction from NRTIs increased reactive oxygen species (ROS) within the affected cell and amplified mitochondrial dysfunction in a feed-forward way (20). We prevented or attenuated NRTI toxicity both in vitro with exogenous metalloporphyrin antioxidants administration and in vivo with genetically engineered murine overexpression of mitochondrially targeted antioxidant enzymes (20,21,41).…”

mentioning

confidence: 97%

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AZT-induced mitochondrial toxicity: an epigenetic paradigm for dysregulation of gene expression through mitochondrial oxidative stress

Koczor

Jing

Fields

et al. 2015

Physiological Genomics

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Koczor CA, Jiao Z, Fields E, Russ R, Ludaway T, Lewis W. AZT-induced mitochondrial toxicity: an epigenetic paradigm for dysregulation of gene expression through mitochondrial oxidative stress. Physiol Genomics 47: 447-454, 2015. First published July 21, 2015 doi:10.1152/physiolgenomics.00045.2015.-Mitochondrial dysfunction causes oxidative stress and cardiomyopathy. Oxidative stress also is a side effect of dideoxynucleoside antiretrovirals (NRTI) and is observed in NRTI-induced cardiomyopathy. We show here that treatment with the NRTI AZT {1-[(2R,4S,5S)-4-azido-5-(hydroxymethyl)oxolan-2-yl]-5-methylpyrimidine-2,4-dione} modulates cardiac gene expression epigenetically through production of mitochondrially derived reactive oxygen species. Transgenic mice with ubiquitous expression of mitochondrially targeted catalase (MCAT) and C57Bl/6 wild-type mice littermates (WT) were administered AZT (0.22 mg/day po, 35 days), and cardiac DNA and mRNA were isolated. In AZT-treated WT, 95 cardiac genes were differentially expressed compared with vehicle-treated WTs. When MCAT mice were treated with AZT, each of those 95 genes reverted toward the expression of vehicle-treated WTs. In AZT-treated WT hearts, Mthfr [5,10-methylenetetrahydrofolate reductase; a critical enzyme in synthesis of methionine cycle intermediates including S-adenosylmethionine (SAM)], was overexpressed. Steady-state abundance of SAM in cardiac extracts from AZT-treated MCAT mice increased 60% above that of vehicle-treated MCAT. No such change occurred in WT. AZT caused hypermethylation (47%) and hypomethylation (53%) of differentially methylated DNA regions in WT cardiac DNA. AZTtreated MCAT heart DNA exhibited greater hypermethylation (91%) and less hypomethylation (9%) compared with vehicle-treated MCAT controls. The gene encoding protein kinase C-␣ displayed multifocal epigenetic regulation caused by oxidative stress. Results show that mitochondrially derived oxidative stress in the heart hinders cardiac DNA methylation, alters steady-state abundance of SAM, alters cardiac gene expression, and promotes characteristic pathophysiological changes of cardiomyopathy. This mechanism for NRTI toxicity offers insight into long-term side effects from these commonly used antiviral agents.

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confidence: 91%

Section: Discussionmentioning

confidence: 97%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 97%

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AZT-induced mitochondrial toxicity: an epigenetic paradigm for dysregulation of gene expression through mitochondrial oxidative stress

Koczor

Jing

Fields

et al. 2015

Physiological Genomics

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“…Animal studies using transgenic mice over-expressing mitochondrially-targeted SOD and catalase have already shown the potential of this strategy, since these transgenic mice were associated with significant reductions in cardiac mitochondrial oxidative stress and improvements in left ventricular function after antiretroviral-induced cardiomyopathy (Kohler et al 2009). Indeed, the development of antioxidants that specifically target the matrix-facing inner surface of the mitochondrial membrane is hypothesised to protect against mitochondrial oxidative damage (Ross et al 2005).…”

Section: Mitochondrially-targeted Antioxidantsmentioning

confidence: 99%