Zhou Xian-Yong, Luo Yu, Zhu Yong-Ming, Liu Zhi-He, Kent Thomas A, Rong Jia-Guo, Li Wei, Qiao Shi-Gang, Li Min, Ni Yong, Ishidoh Kazumi, Zhang Hui-Ling
Jiangsu Key Laboratory of Translational Research and Therapy for Neuro-Psycho-Diseases, College of Pharmaceutical Science; Department of Pharmacology and Laboratory of Cerebrovascular Pharmacology; Jiangsu Key Laboratory of Preventive and Translational Medicine for Geriatric Diseases, School of Public Health, Soochow University, Suzhou, China.
Guangzhou Institute of Traumatic Surgery, Guangzhou Red Cross Hospital, Medical College, Jinan University, Guangzhou, China.
Cell Death Dis. 2017 Feb 16;8(2):e2618. doi: 10.1038/cddis.2017.34.
Our previous study and others have demonstrated that autophagy is activated in ischemic astrocytes and contributes to astrocytic cell death. However, the mechanisms of ischemia-induced autophagy remain largely unknown. In this study, we established a rat's model of permanent middle cerebral artery occlusion (pMCAO) and an in vitro oxygen and glucose deprivation (OGD) model. Autophagy was inhibited by either pharmacological treatment with 3-methyladenine (3-MA) and wortmannin (Wort) or genetic treatment with knockdown of Atg5 in primary cultured astrocytes and knockout of Atg5 in mouse embryonic fibroblast (MEF) cells, respectively. We found that pharmacological or genetic inhibition of autophagy reversed pMCAO or OGD-induced increase in LC3-II, active cathepsin B and L, tBid, active caspase-3 and cytoplastic cytochrome c (Cyt-c), and suppressed the injury-induced reduction in mitochondrial Cyt-c in ischemic cortex, in injured astrocytes and MEF cells. Immunofluorescence analysis showed that 3-MA or Wort treatment reversed OGD-induced release of cathepsin B and L from the lysosome to the cytoplasm and activation of caspase-3 in the astrocytes. Furthermore, treatment of 3-MA or Wort decreased OGD-induced increase in lysosomal membrane permeability and enhanced OGD-induced upregulation of lysosomal heat shock protein 70.1B (Hsp70.1B) in astrocytes. Inhibition of autophagy by 3-MA or Wort reduced infarction volume in rats and protected OGD-induced astrocytic cell injury. A non-selective caspase inhibitor z-VAD-fmk or a specific caspase-3 inhibitor Q-DEVD-OPh also rescued OGD-induced astrocytic cell injury. In conclusion, our presenting data suggest that inhibition of autophagy blocks cathepsins-tBid-mitochondrial apoptotic signaling pathway via stabilization of lysosomal membranes, possibly due to upregulation of the lysosomal Hsp70.1B in ischemic astrocytes.
我们之前的研究及其他研究表明,自噬在缺血性星形胶质细胞中被激活,并导致星形胶质细胞死亡。然而,缺血诱导自噬的机制仍 largely 未知。在本研究中,我们建立了大鼠永久性大脑中动脉闭塞(pMCAO)模型和体外氧糖剥夺(OGD)模型。分别通过用 3 - 甲基腺嘌呤(3 - MA)和渥曼青霉素(Wort)进行药物处理,或在原代培养的星形胶质细胞中敲低 Atg5 以及在小鼠胚胎成纤维细胞(MEF)中敲除 Atg5 进行基因处理来抑制自噬。我们发现,自噬的药物或基因抑制可逆转 pMCAO 或 OGD 诱导的 LC3 - II、活性组织蛋白酶 B 和 L、tBid、活性半胱天冬酶 - 3 和细胞质细胞色素 c(Cyt - c)的增加,并抑制缺血皮质、损伤的星形胶质细胞和 MEF 细胞中损伤诱导的线粒体 Cyt - c 减少。免疫荧光分析表明,3 - MA 或 Wort 处理可逆转 OGD 诱导的组织蛋白酶 B 和 L 从溶酶体释放到细胞质以及星形胶质细胞中半胱天冬酶 - 3 的激活。此外,3 - MA 或 Wort 处理可降低 OGD 诱导的溶酶体膜通透性增加,并增强 OGD 诱导的星形胶质细胞中溶酶体热休克蛋白 70.1B(Hsp70.1B)的上调。3 - MA 或 Wort 抑制自噬可减少大鼠梗死体积,并保护 OGD 诱导的星形胶质细胞损伤。非选择性半胱天冬酶抑制剂 z - VAD - fmk 或特异性半胱天冬酶 - 3 抑制剂 Q - DEVD - OPh 也可挽救 OGD 诱导的星形胶质细胞损伤。总之,我们目前的数据表明,自噬抑制通过稳定溶酶体膜来阻断组织蛋白酶 - tBid - 线粒体凋亡信号通路,这可能是由于缺血性星形胶质细胞中溶酶体 Hsp70.1B 的上调所致。
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