抑制动力相关蛋白1可保护糖尿病小鼠免受心肌缺血再灌注损伤。

Inhibition of dynamin-related protein 1 protects against myocardial ischemia-reperfusion injury in diabetic mice.

作者信息

Ding Mingge, Dong Qianqian, Liu Zhenghua, Liu Zheng, Qu Yinxian, Li Xing, Huo Cong, Jia Xin, Fu Feng, Wang Xiaoming

机构信息

Department of Geriatrics, Xi'an Central Hospital, Xi'an, 710003, China.

Department of Geriatrics, Xijing Hospital, Fourth Military Medical University, 15 Changlexi Road, Xi'an, 710032, China.

出版信息

Cardiovasc Diabetol. 2017 Feb 7;16(1):19. doi: 10.1186/s12933-017-0501-2.

DOI:10.1186/s12933-017-0501-2

PMID:28173848

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5297196/

Abstract

BACKGROUND

Many cardioprotective pharmacological agents failed to exert their protective effects in diabetic hearts subjected to myocardial ischemia/reperfusion (MI/R). Identify the molecular basis linking diabetes with MI/R injury is scientifically important and may provide effective therapeutic approaches. Dynamin-related protein 1 (Drp1)-mediated mitochondrial fission plays an important role in MI/R injury under non-diabetic conditions. Importantly, recent studies indicated that Drp1-mediated mitochondrial fission is enhanced in the myocardium of diabetic mice. The above evidences suggested that Drp1 may be one critical molecule linking diabetes with MI/R injury. We hypothesized that inhibition of Drp1 may be effective to reduce MI/R injury in diabetic hearts.

METHODS

High-fat diet and streptozotocin-induced diabetic mice were subjected to MI/R or sham operation. Mdivi-1 (1.2 mg/kg), a small molecule inhibitor of Drp1 or vehicle was administrated 15 min before the onset of reperfusion. Outcome measures included mitochondrial morphology, mitochondrial function, myocardial injury, cardiac function and oxidative stress.

RESULTS

Mitochondrial fission was significantly increased following MI/R as evidenced by enhanced translocation of Drp1 to mitochondria and decreased mitochondrial size. Delivery of Mdivi-1 into diabetic mice markedly inhibited Drp1 translocation to the mitochondria and reduced mitochondrial fission following MI/R. Inhibition of Drp1 in diabetic hearts improved mitochondrial function and cardiac function following MI/R. Moreover, inhibition of Drp1 reduced myocardial infarct size and serum cardiac troponin I and lactate dehydrogenase activities. These cardioprotective effects were associated with decreased cardiomyocyte apoptosis and malondialdehyde production and increased activities of antioxidant enzyme manganese superoxide dismutase.

CONCLUSIONS

Pharmacological inhibition of Drp1 prevents mitochondrial fission and reduces MI/R injury in diabetic mice. The findings suggest Drp1 may be a potential novel therapeutic target for diabetic cardiac complications.

摘要

背景

许多心脏保护药物在糖尿病心脏遭受心肌缺血/再灌注（MI/R）时未能发挥其保护作用。确定将糖尿病与MI/R损伤联系起来的分子基础具有重要的科学意义，并可能提供有效的治疗方法。动力相关蛋白1（Drp1）介导的线粒体分裂在非糖尿病条件下的MI/R损伤中起重要作用。重要的是，最近的研究表明，Drp1介导的线粒体分裂在糖尿病小鼠心肌中增强。上述证据表明，Drp1可能是将糖尿病与MI/R损伤联系起来的关键分子之一。我们假设抑制Drp1可能有效减少糖尿病心脏中的MI/R损伤。

方法

采用高脂饮食和链脲佐菌素诱导的糖尿病小鼠进行MI/R或假手术。在再灌注开始前15分钟给予Drp1的小分子抑制剂Mdivi-1（1.2mg/kg）或赋形剂。观察指标包括线粒体形态、线粒体功能、心肌损伤、心功能和氧化应激。

结果

MI/R后线粒体分裂显著增加，表现为Drp1向线粒体的转位增强和线粒体大小减小。将Mdivi-1给予糖尿病小鼠可显著抑制Drp1向线粒体的转位，并减少MI/R后的线粒体分裂。抑制糖尿病心脏中的Drp1可改善MI/R后的线粒体功能和心功能。此外，抑制Drp1可减小心肌梗死面积，降低血清心肌肌钙蛋白I和乳酸脱氢酶活性。这些心脏保护作用与心肌细胞凋亡减少、丙二醛生成减少以及抗氧化酶锰超氧化物歧化酶活性增加有关。