شکوهی ثابت, نیما ، آتش بار, سامان ، محمدخانلو, الهام ، کهریزی, فرزاد ، سلیمی, احمد (1399) کورکومین با سرکوب استرس اکسیداتیو و جلوگیری از اختلال عملکرد میتوکندری در میتوکندری قلب ، سمیت ناشی از بواسیزوماب را کاهش می دهد. Naunyn-Schmiedeberg's Archives of Pharmacology ــ 393 (8). ص.ص.1447-1457. شاپا 0028-1298
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آدرس اینترنتی رسمی : https://link.springer.com/article/10.1007/s00210-0...
عنوان انگليسی
Curcumin attenuates bevacizumab-induced toxicity via suppressing oxidative stress and preventing mitochondrial dysfunction in heart mitochondria
خلاصه انگلیسی
Heart failure was subsequently noted in 2–4% of patients on bevacizumab (BEV). Whereas mitochondria play an important role in myocardial tissue homeostasis, deterioration in mitochondrial function will eventually lead to cardiomyocyte cell death and consequently cardiovascular dysfunction. Therefore, the aim of our study is to search the effects of BEV on isolated rat heart mitochondria and cardiomyocytes, and survey the effect of curcumin as a mitochondrial protective and cardioprotective agent. Rat heart mitochondria and cardiomyocytes were isolated from adult rat heart ventricular. By using biochemical and flow cytometry evaluations, the parameters of mitochondrial toxicity including succinate dehydrogenase (SDH) activity, mitochondrial swelling, mitochondrial membrane potential (MMP) collapse, reactive oxygen species (ROS) formation and lipid peroxidation (LP), and cellular assays such as cytotoxicity and MMP collapse were evaluated. Results revealed that BEV (up to 50μg/ml) induced a concentration- and time-dependent rise in mitochondrial ROS formation, MMP collapse, mitochondrial swelling, LP, and inhibition of SDH in rat heart mitochondria. Our results showed that curcumin (10–100 μM) significantly ameliorated BEV-induced mitochondrial toxicities. Also, our results in cellular assays confirmed amelioration effect of curcumin against BEV toxicity. These results indicate that the cardiotoxic effects of BEV are associated with mitochondrial dysfunction and ROS formation, which finally ends in MMP collapse and mitochondrial swelling as the “point of no return” in the cascade of events leading to apoptosis. Also, results of this study suggest that probably the combination therapy of BEV and curcumin could decrease mitochondrial effects of this drug.
| نوع سند : | مقاله |
|---|---|
| زبان سند : | انگلیسی |
| نویسنده اول : | نیما شکوهی ثابت |
| نویسنده : | سامان آتش بار |
| نویسنده : | الهام محمدخانلو |
| نویسنده : | فرزاد کهریزی |
| نویسنده مسئول : | احمد سلیمی |
| ضریب تاثیر و نمایه مجلات: | IF: 3 Indexed in: ISI, PubMed/Medline, Scopus, Embase |
| کلیدواژه ها (انگلیسی): | Cardiotoxicity; Mitochondria; Heart failure; Cardioprotective |
| موضوعات : | QV فارماکولوژی > QV 600 سم شناسی |
| بخش های دانشگاهی : | دانشکده داروسازی > بخش سم شناسی |
| کد شناسایی : | 12773 |
| ارائه شده توسط : | دکتر احمد سلیمی |
| ارائه شده در تاریخ : | 26 اسفند 1398 12:27 |
| آخرین تغییر : | 25 فروردین 1401 09:31 |
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