Journal
MITOCHONDRION
Volume 20, Issue -, Pages 22-33Publisher
ELSEVIER SCI LTD
DOI: 10.1016/j.mito.2014.10.008
Keywords
Cardioprotection; Adriamycin; Exercise; Bioenergetics; Oxidative damage
Categories
Funding
- Portuguese Foundation for Science and Technology (FTC)
- Muscletech Network [MTN20100101]
- Plan Nacional [I D I DEP2010-22205-C02-01]
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Doxorubicin (DOX) is an anti-cancer agent whose clinical usage results in a cumulative and dose-dependent cardiotoxicity. We have previously shown that exercise performed prior to DOX treatment reduces the resulting cardiac(mito) toxicity. We sought to determine the effects on cardiac mitochondrial toxicity of two distinct chronic exercise models (endurance treadmill training-TM and voluntary free-wheel activity-FW) when used prior and during DOX treatment. Male-young Sprague Dawley rats were divided into six groups (n = 6 per group): SAL + SED (saline sedentary), SAL + TM (12-weeks TM), SAL + FW (12-weeks FW), DOX + SED (7-weeks of chronic DOX treatment 2 mg/kg per week), DOX + TM and DOX + FW. DOX administration started 5 weeks after the beginning of the exercise protocol. Heart mitochondrial ultrastructural alterations, mitochondrial function (oxygen consumption and membrane potential), semi-quantification of oxidative phosphorylation (OXPHOS) proteins and their in-gel activity, as well as proteins involved in mitochondrial oxidative stress (SIRT3, p66shc and UCP2), biogenesis (PGC1 alpha and TFAM), acetylation and markers for oxidative damage (carbonyl groups, MDA, - SH, aconitase, Mn-SOD activity) were evaluated. DOX treatment resulted in ultrastructural and functional alterations and decreased OXPHOS. Moreover, DOX decreased complex I activity and content, mitochondria( biogenesis (TFAM), increased acetylation and oxidative stress. TM and FW prevented DOX-induced alteration in OXPHOS, the increase in oxidative stress, the decrease in complex V activity and in complex I activity and content. DOX-induced decreases in TFAM and SIRT3 content were prevented by TM only. Both chronic models of physical exercise performed before and during the course of sub-chronic DOX treatment translated into an improved mitochondrial bioenergetic fitness, which may result in part from the prevention of mitochondrial oxidative stress and damage. (C) 2014 Elsevier BM. and Mitochondria Research Society. All rights reserved.
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