Apelin-13 通过时间依赖性抑制 ER 依赖性凋亡途径保护心脏免受缺血再灌注损伤。
Apelin-13 protects the heart against ischemia-reperfusion injury through inhibition of ER-dependent apoptotic pathways in a time-dependent fashion.
机构信息
Division of Cardiology, Shanghai Sixth Hospital, Shanghai Jiao Tong University School of Medicine, State Key Discipline Cardiology, Shanghai, People's Republic of China.
出版信息
Am J Physiol Heart Circ Physiol. 2011 Oct;301(4):H1471-86. doi: 10.1152/ajpheart.00097.2011. Epub 2011 Jul 29.
Endoplasmic reticulum (ER) stress is activated during and contributes to ischemia-reperfusion (I/R) injury. Attenuation of ER stress-induced apoptosis protects the heart against I/R injury. Using apelin, a ligand used to activate the apelin APJ receptor, which is known to be cardioprotective, this study was designed to investigate 1) the time course of changes in I/R injury after ER stress; 2) whether apelin infusion protects the heart against I/R injury via modulation of ER stress-dependent apoptosis signaling pathways; and 3) how phosphatidylinositol 3-kinase (PI3K)/Akt, endothelial nitric oxide synthase (eNOS), AMP-activated protein kinase (AMPK), and ERK activation are involved in the protection offered by apelin treatment. The results showed that, using an in vivo rat I/R model induced by 30 min of ischemia followed by reperfusion, infarct size (IS) increased from 2 h of reperfusion (34.85 ± 2.14%) to 12 h of reperfusion (48.98 ± 3.35, P < 0.05), which was associated with an abrupt increase in ER stress-dependent apoptosis activation, as evidenced by increased CCAAT/enhancer-binding protein homologous protein (CHOP), caspase-12, and JNK activation (CHOP: 2.49-fold increase, caspase-12: 2.09-fold increase, and JNK: 3.38-fold increase, P < 0.05, respectively). Administration of apelin at 1 μg/kg not only completely abolished the activation of ER stress-induced apoptosis signaling pathways at 2 h of reperfusion but also significantly attenuated time-related changes at 24 h of reperfusion. Using pharmacological inhibition, we also demonstrated that PI3K/Akt, AMPK, and ERK activation were involved in the protection against I/R injury via inhibition of ER stress-dependent apoptosis activation. In contrast, although eNOS activation played a role in decreasing IS at 2 h of reperfusion, it failed to modify either IS or ER stress-induced apoptosis signaling pathways at 24 h after reperfusion.
内质网(ER)应激在缺血再灌注(I/R)损伤期间被激活,并有助于其发生。减轻 ER 应激诱导的细胞凋亡可保护心脏免受 I/R 损伤。本研究使用了一种名为 apelin 的配体,它可以激活已知具有心脏保护作用的 apelin APJ 受体。该研究旨在探讨:1)ER 应激后 I/R 损伤变化的时间过程;2)apelin 输注是否通过调节 ER 应激依赖性细胞凋亡信号通路来保护心脏免受 I/R 损伤;3)磷脂酰肌醇 3-激酶(PI3K)/Akt、内皮型一氧化氮合酶(eNOS)、AMP 激活的蛋白激酶(AMPK)和细胞外信号调节激酶(ERK)的激活如何参与 apelin 治疗提供的保护作用。结果表明,在 30 分钟缺血后再灌注诱导的体内大鼠 I/R 模型中,梗死面积(IS)从再灌注 2 小时(34.85±2.14%)增加到再灌注 12 小时(48.98±3.35,P<0.05),这与 ER 应激依赖性细胞凋亡激活的急剧增加有关,证据是 CCAAT/增强子结合蛋白同源蛋白(CHOP)、半胱天冬酶-12 和 JNK 激活增加(CHOP:增加 2.49 倍,半胱天冬酶-12:增加 2.09 倍,JNK:增加 3.38 倍,P<0.05)。给予 1μg/kg 的 apelin 不仅完全消除了再灌注 2 小时时 ER 应激诱导的细胞凋亡信号通路的激活,而且还显著减轻了再灌注 24 小时时的时间相关变化。通过药理抑制,我们还证明 PI3K/Akt、AMPK 和 ERK 的激活通过抑制 ER 应激依赖性细胞凋亡激活参与了对 I/R 损伤的保护作用。相比之下,尽管 eNOS 激活在再灌注 2 小时时减少了 IS,但它未能在再灌注后 24 小时时改变 IS 或 ER 应激诱导的细胞凋亡信号通路。
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