Katepsin B İnhibitörü olan CA074'ün Serebral İskemi Modelinde Apoptoz ve Hücre Ölümü Üzerine Etkisi

Emre ÖZKARA, Ramazan DURMAZ, Zühtü ÖZBEK, Hilmi ÖZDEN, Güngör KANBAK, Kubilay UZUNER
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Abstract

Lysosomes and cathepsins, the most common hydrolytic enzymes in lysosomes, are available in the different models of cell death as necrosis and apoptosis. This study investigated the effect of cathepsin B-selective inhibitor CA-074 on apoptotic and necrotic neuronal cell death. Focal cerebral ischemia which has been formed by occlusion of the three-vessel consisting permanent middle cerebral artery occlusion and temporary bilateral common carotid artery occlusion for 60 minutes was selected as ischemia model. Two sets of rats were used in this study. The rats in the first set were used formeasurement of sulfhydryl groups in the lysosomal membrane, lysosomal integrity, cathepsins B and L activities and caspase-3 activity. The rats in the second set were used as histological study including "hematoxylin and eosin" for the detection of necrotic neuronal deathand "TUNEL" staining for the detection of apoptotic neuronal death. 4 mg/kg CA-074 was administered intravenouslyin the treatment group. CA-074 has substantially reduced levels of cathepsins B and L compared to ischemia and solvent groups (respectively, p<0.05 and p<0.01). Similarly, CA-074 has reduced increase in caspase-3 activity compared to ischemia and solvent groups (p<0.05). While the number of eosinophilic (necrotic) and apoptotic neurons has highly increased in post-ischemic cerebral tissue in middle cerebral artery feeding area (p<0.001), CA-074 could only reduce significantly the number of apoptotic neurons (p<0.05). CA-074 has reduced apoptotic neuronal death by inhibiting caspase and cathepsin activity. It may be useful that CA074 is used with other therapeutic drugs in stroke patients.
Cathepsin B抑制剂CA074对脑缺血模型中细胞凋亡和细胞死亡的影响
溶酶体和组织蛋白酶是溶酶体中最常见的水解酶,可用于不同的细胞死亡模式,如坏死和凋亡。本研究探讨组织蛋白酶b选择性抑制剂CA-074对凋亡和坏死神经元细胞死亡的影响。选择永久性大脑中动脉和暂时性双侧颈总动脉三支血管闭塞60分钟形成局灶性脑缺血作为缺血模型。本研究采用两组大鼠。测定第一组大鼠溶酶体膜巯基、溶酶体完整性、组织蛋白酶B、L活性和caspase-3活性。第二组大鼠采用“苏木精伊红”染色法检测坏死神经元死亡,“TUNEL”染色法检测凋亡神经元死亡。治疗组静脉滴注CA-074 4 mg/kg。与缺血组和溶剂组相比,CA-074显著降低组织蛋白酶B和L的水平(分别为p<0.05和p<0.01)。同样,与缺血组和溶剂组相比,CA-074减少了caspase-3活性的增加(p<0.05)。大脑中动脉供血区缺血后脑组织中嗜酸性(坏死)和凋亡神经元数量大量增加(p<0.001), CA-074仅能显著减少凋亡神经元数量(p<0.05)。CA-074通过抑制caspase和组织蛋白酶活性减少凋亡神经元死亡。CA074与其他治疗药物一起用于脑卒中患者可能是有用的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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