Institute of Basic Medical Sciences, Xiyuan Hospital of China Academy of Chinese Medical Sciences, Beijing, 100091, China.
Laboratory of Cardiovascular Diseases, Xiyuan Hospital of China Academy of Chinese Medical Sciences, Beijing, 100091, China; National Clinical Research Center for Chinese Medicine Cardiology, Xiyuan Hospital, Beijing, 100091, China.
J Ethnopharmacol. 2024 Jan 30;319(Pt 3):117338. doi: 10.1016/j.jep.2023.117338. Epub 2023 Oct 27.
Cardiovascular disease (CVD) and fatigue are two common diseases endangering human life and health that may interact and reinforce one another. Myocardial infarction survivors frequently experience fatigue, and acute myocardial infarction (AMI) is one of the most common cardiovascular diseases that cause fatigue-induced sudden death. Sheng Mai Yin (SMY), a Chinese medicine prescription, is traditionally used for the treatment of diabetes and cardiovascular disease, and has been demonstrated to reduce fatigue and safeguard cardiac function.
This study aims to investigate the effects and underlying mechanisms of SMY in treating fatigue and AMI.
The pharmacological mechanisms of SMY in treating fatigue and AMI were predicted by bioinformatics and network pharmacology methods. After administering SMY at high, medium and low doses, the swimming time to exhaustion, hemoglobin level, serological parameters and hypoxia tolerance time were detected in C57BL/6N mice, and the left ventricular ejection fractions (LVEF), left ventricular fractional shortening (LVFS), grasp strength, cardiac histopathology, serological parameters and the expression of PINK1 and Parkin proteins were examined in Wistar rats.
371 core targets for SMY and 282 disease targets for fatigue and AMI were obtained using bioinformatics and network pharmacology methods. Enrichment analysis of target genes revealed that SMY might interfere with fatigue and AMI through biological processes such as mitochondrial autophagy, apoptosis, and oxidative stress. For in vivo experiments, SMY showed significant anti-fatigue and hypoxia tolerance effects in mice; It also improved the cardiac function and grasp strength, decreased their cardiac index, myocardial injury and fibrosis degree, and induced serological parameters levels and the expression of PTEN-induced putative kinase 1 (PINK1) and Parkin proteins in myocardium, suggesting that SMY may exert cardioprotective effects in a joint rat model of fatigue and AMI by inhibiting excessive mitochondrial autophagy.
This study revealed the anti-fatigue, anti-hypoxia and cardioprotective effects of SMY in a joint model of fatigue-AMI, and the pharmacological mechanism may be related to the inhibition of mitochondrial autophagy in cardiomyocytes through the PINK1/Parkin pathway. The discoveries may provide new ideas for the mechanism study of traditional Chinese medicine, especially complex prescriptions, in treating fatigue and AMI.
心血管疾病 (CVD) 和疲劳是两种危害人类生命和健康的常见疾病,它们可能相互作用并相互加强。心肌梗死幸存者经常感到疲劳,而急性心肌梗死 (AMI) 是最常见的心血管疾病之一,可导致疲劳引起的猝死。生脉饮 (SMY) 是一种中药方剂,传统上用于治疗糖尿病和心血管疾病,已被证明可减轻疲劳并保护心脏功能。
本研究旨在探讨 SMY 治疗疲劳和 AMI 的作用及机制。
采用生物信息学和网络药理学方法预测 SMY 治疗疲劳和 AMI 的药理机制。给予高、中、低剂量 SMY 后,检测 C57BL/6N 小鼠的游泳至力竭时间、血红蛋白水平、血清学参数和耐缺氧时间,检测 Wistar 大鼠的左心室射血分数 (LVEF)、左心室缩短分数 (LVFS)、握力、心脏组织病理学、血清学参数和 PINK1 和 Parkin 蛋白的表达。
采用生物信息学和网络药理学方法获得了 371 个 SMY 核心靶点和 282 个疲劳和 AMI 疾病靶点。靶基因富集分析表明,SMY 可能通过线粒体自噬、细胞凋亡和氧化应激等生物学过程干预疲劳和 AMI。体内实验结果显示,SMY 对小鼠有明显的抗疲劳和耐缺氧作用;还改善了心脏功能和握力,降低了心脏指数、心肌损伤和纤维化程度,诱导了血清学参数水平和心肌中 PTEN 诱导的假定激酶 1 (PINK1) 和 Parkin 蛋白的表达,表明 SMY 可能通过抑制过度的线粒体自噬在疲劳-AMI 联合大鼠模型中发挥心脏保护作用。
本研究揭示了 SMY 在疲劳-AMI 联合模型中的抗疲劳、抗缺氧和心脏保护作用,其药理机制可能与通过 PINK1/Parkin 通路抑制心肌细胞中线粒体自噬有关。这些发现可能为中药,特别是复杂方剂治疗疲劳和 AMI 的机制研究提供新的思路。
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