Huang Ling, Dai Kai, Chen Manhua, Zhou Wenping, Wang Xiaoling, Chen Jing, Zhou Wei
Department of Cardiology, The Central Hospital of Wuhan, Wuhan, China
Department of Infectious Diseases, Renmin Hospital of Wuhan University, Wuhan, China.
J Cardiovasc Pharmacol Ther. 2016 Jan;21(1):70-81. doi: 10.1177/1074248415581177. Epub 2015 Apr 13.
Myocardial ischemia has become one of the main causes of sudden cardiac death worldwide. Autophagy has been demonstrated to protect cardiomyocytes from ischemia/reperfusion (I/R)-induced damage. A novel small molecule compound 2-Chloro-5-[[5-[[5-(4,5-Dimethyl-2-nitrophenyl)-2-furanyl]methylene]-4,5-dihydro-4-oxo-2-thiazolyl]amino]benzoic acid (PT1) has been previously shown to specifically activate 5'-adenosine monophosphate-activated protein kinase (AMPK). Because AMPK activation effectively induces autophagy, we tested the protective efficacy of PT1 on cardiomyocytes after oxygen glucose deprivation/reoxygenation (OGD/R) in vitro. Mouse neonatal cardiomyocytes were treated with PT1 after OGD/R. 3-[4-(1,3-benzodioxol-5-yl)-2-oxo-3-buten-1-yl]-3-hydroxy-1,3-dihydro-2H-indol-2-one (3HOI-BA-01), a novel small compound showing potent inhibitory effect on mammalian target of rapamycin (mTOR) activation, was also tested for its cardioprotective effect, based on the established relationship between mTOR signaling and autophagy. Cell survival and autophagy-related signal pathways were examined after treatment with these agents. Our data indicate that both PT1 and 3HOI-BA-01 enhance cell survival after OGD/R. As expected, both PT1 and 3HOI-BA-01 induced autophagy in cardiomyocytes through activating AMPK pathway and inhibiting mTOR signaling, respectively. Induction of autophagy by PT1 and 3HOI-BA-01 was responsible for their cardioprotective effect, since inhibition of autophagy abolished the protective efficacy. Furthermore, simultaneous administration of PT1 and 3HOI-BA-01 profoundly upregulated autophagy after OGD/R and significantly promoted survival of cardiomyocytes. In vivo administration of PT1 and 3HOI-BA-01 in a murine myocardial (I/R injury model remarkably reduced infarct size and induced autophagy. Taken together, our research suggests that PT1 and 3HOI-BA-01 could be promising therapeutic agents for myocardial ischemia.
心肌缺血已成为全球心脏性猝死的主要原因之一。自噬已被证明可保护心肌细胞免受缺血/再灌注(I/R)诱导的损伤。一种新型小分子化合物2-氯-5-[[5-[[5-(4,5-二甲基-2-硝基苯基)-2-呋喃基]亚甲基]-4,5-二氢-4-氧代-2-噻唑基]氨基]苯甲酸(PT1)先前已被证明可特异性激活5'-腺苷单磷酸激活蛋白激酶(AMPK)。由于AMPK激活可有效诱导自噬,我们在体外测试了PT1对氧糖剥夺/复氧(OGD/R)后心肌细胞的保护作用。OGD/R后用PT1处理小鼠新生心肌细胞。基于雷帕霉素哺乳动物靶点(mTOR)信号与自噬之间已确立的关系,还测试了一种对mTOR激活具有强效抑制作用的新型小分子化合物3-[4-(1,3-苯并二氧杂环戊烯-5-基)-2-氧代-3-丁烯-1-基]-3-羟基-1,3-二氢-2H-吲哚-2-酮(3HOI-BA-01)的心脏保护作用。用这些药物处理后检测细胞存活和自噬相关信号通路。我们的数据表明,PT1和3HOI-BA-01均可提高OGD/R后的细胞存活率。正如预期的那样,PT1和3HOI-BA-01分别通过激活AMPK途径和抑制mTOR信号在心肌细胞中诱导自噬。PT1和3HOI-BA-诱导的自噬是它们心脏保护作用的原因,因为抑制自噬消除了保护作用。此外,同时给予PT1和3HOI-BA-01可在OGD/R后显著上调自噬并显著促进心肌细胞存活。在小鼠心肌(I/R)损伤模型中体内给予PT1和3HOI-BA-01可显著减小梗死面积并诱导自噬。综上所述,我们的研究表明PT1和3HOI-BA-01可能是治疗心肌缺血的有前途的治疗药物。
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