Concepedia

Publication | Closed Access

Hesperetin ameliorates ischemia/hypoxia‐induced myocardium injury via inhibition of oxidative stress, apoptosis, and regulation of Ca<sup>2+</sup> homeostasis

DOI

15

Citations

49

References

2022

Year

Panpan Liu, Jian Chen, Jiaying Qi, Miaomiao Liu, Muqing Zhang, Yucong Xue, Li Li, Yanshuang Liu, Jing Shi, Yixin Zhang,
Phytotherapy Research

Abstract

Ischemia/hypoxia (I/H)-induced myocardial injury has a large burden worldwide. Hesperetin (HSP) has a cardioprotective effect, but the molecular mechanism underlying this is not clearly established. Here, we focused on the protective mechanisms of HSP against I/H-induced myocardium injury. H9c2 cardiomyocytes were challenged with CoCl<sub>2</sub> for 22 h to imitate hypoxia after treatment groups received HSP for 4 h. The viability of H9c2 cardiomyocytes was evaluated, and cardiac function indices, reactive oxygen species, apoptosis, mitochondrial membrane potential (MMP), and intracellular Ca<sup>2+</sup> concentration ([Ca<sup>2+</sup> ]<sub>i</sub> ) were measured. L-type Ca<sup>2+</sup> current (I<sub>Ca-L</sub> ), myocardial contraction, and Ca<sup>2+</sup> transients in isolated ventricular myocytes were also recorded. We found that HSP significantly increased the cell viability, and MMP while significantly decreasing cardiac impairment, oxidative stress, apoptosis, and [Ca<sup>2+</sup> ]<sub>i</sub> caused by CoCl<sub>2</sub> . Furthermore, HSP markedly attenuated I<sub>Ca-L</sub> , myocardial contraction, and Ca<sup>2+</sup> transients in a concentration-dependent manner. Our findings suggest a protective mechanism of HSP on I/H-induced myocardium injury by restoring oxidative balance, inhibiting apoptosis, improving mitochondrial function, and reducing Ca<sup>2+</sup> influx via L-type Ca<sup>2+</sup> channels (LTCCs). These data provide a new direction for HSP applied research as a LTCC inhibitor against I/H-induced myocardium injury.

References

YearCitations

Page 1