. 2019 Sep 10;517(1):111-117.

doi: 10.1016/j.bbrc.2019.07.029. Epub 2019 Jul 12.

Dosing depending on SIRT3 activity attenuates doxorubicin-induced cardiotoxicity via elevated tolerance against mitochondrial dysfunction and oxidative stress

Na Yang¹, Haoyue Ma², Zhou Jiang³, Lihong Niu⁴, Xinshang Zhang⁴, Yanyou Liu³, Yuhui Wang³, Shuting Cheng³, Yan Deng⁴, Hongyi Qi⁵, Zhengrong Wang⁶

Affiliations

¹ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China; Academy of Medical Sciences & Sichuan Provincial People's Hospital, 32nd West Second Section, First Ring Road, Chengdu, Sichuan, 610072, China.
² College of Pharmaceutical Sciences, Southwest University, 2 Tiansheng Road, Beibei District, Chongqing, 400716, China.
³ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China.
⁴ Academy of Medical Sciences & Sichuan Provincial People's Hospital, 32nd West Second Section, First Ring Road, Chengdu, Sichuan, 610072, China.
⁵ College of Pharmaceutical Sciences, Southwest University, 2 Tiansheng Road, Beibei District, Chongqing, 400716, China. Electronic address: hongyiqi@swu.edu.cn.
⁶ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China. Electronic address: wangzhengrong@126.com.

PMID: 31303273
DOI: 10.1016/j.bbrc.2019.07.029

Dosing depending on SIRT3 activity attenuates doxorubicin-induced cardiotoxicity via elevated tolerance against mitochondrial dysfunction and oxidative stress

Na Yang et al. Biochem Biophys Res Commun. 2019.

. 2019 Sep 10;517(1):111-117.

doi: 10.1016/j.bbrc.2019.07.029. Epub 2019 Jul 12.

Authors

Na Yang¹, Haoyue Ma², Zhou Jiang³, Lihong Niu⁴, Xinshang Zhang⁴, Yanyou Liu³, Yuhui Wang³, Shuting Cheng³, Yan Deng⁴, Hongyi Qi⁵, Zhengrong Wang⁶

Affiliations

¹ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China; Academy of Medical Sciences & Sichuan Provincial People's Hospital, 32nd West Second Section, First Ring Road, Chengdu, Sichuan, 610072, China.
² College of Pharmaceutical Sciences, Southwest University, 2 Tiansheng Road, Beibei District, Chongqing, 400716, China.
³ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China.
⁴ Academy of Medical Sciences & Sichuan Provincial People's Hospital, 32nd West Second Section, First Ring Road, Chengdu, Sichuan, 610072, China.
⁵ College of Pharmaceutical Sciences, Southwest University, 2 Tiansheng Road, Beibei District, Chongqing, 400716, China. Electronic address: hongyiqi@swu.edu.cn.
⁶ Health Ministry Key Laboratory of Chronobiology, College of Basic Medicine and Forensic Medicine, Sichuan University, 9th Middle Segment, 17 Renmin South Road, Chengdu, Sichuan, 610041, China. Electronic address: wangzhengrong@126.com.

PMID: 31303273
DOI: 10.1016/j.bbrc.2019.07.029

Abstract

Doxorubicin (DOX) is a potent anti-neoplastic agent with cumulative cardiotoxicity. DOX-induced cardiotoxicity has been shown to depend on the different dosing times. However, the basis for determining the dosing time to minimize DOX-induced cardiotoxicity and the underlying mechanisms remain incompletely understood. Here we first showed that SIRT3, the major mitochondrial deacetylase, is negatively correlated to DOX-induced cardiotoxicity through the regulation of ATP production, mitochondrial membrane potential (MMP) level and ROS level in human pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs). Then, we used in vivo experiments to demonstrate that DOX significantly reduced the SIRT3 expression and the SIRT3 activity as reflected by the increased Ac^K68MnSOD/MnSOD ratio in rats after six weeks of treatment. Notably, the activity of SIRT3 had an obvious diurnal rhythm pattern in the myocardium of healthy rats. More importantly, an obvious lower Ac^K68MnSOD/MnSOD ratio was observed in rat hearts with DOX administrated at Zeitgeber time (ZT) 9 (ZT 0 was the time lights were turned on) than ZT1, which represent the peak and trough of SIRT3 activity. Moreover, DOX ZT9 reduced the body weight loss, extended the survival period, improved the heart function and alleviated the myocardial lesions compared to DOX ZT1. Mechanistic investigations demonstrated that DOX ZT1 significantly reduced ATP production, oxygen consumption rate (OCR) at various respiration states, MMP level and MnSOD activity and enhanced the H₂O₂ level compared with CON ZT1, whereas there was no significant effect for DOX ZT9 compared with CON ZT9. Taken together, dosing at the peak time of SIRT3 activity reduced DOX-induced cardiotoxicity, which may be related to the increased endogenous tolerance against the mitochondrial dysfunction and oxidative stress caused by DOX.

Keywords: Biological rhythm; Cardiotoxicity; Doxorubicin; Mitochondrial dysfunction; Oxidative stress; Sirtuin 3.

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Dosing depending on SIRT3 activity attenuates doxorubicin-induced cardiotoxicity via elevated tolerance against mitochondrial dysfunction and oxidative stress

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Dosing depending on SIRT3 activity attenuates doxorubicin-induced cardiotoxicity via elevated tolerance against mitochondrial dysfunction and oxidative stress

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