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首页> 外文期刊>Journal of Clinical and Diagnostic Research >Myocardial Salvaging Effects of Berberine in Experimental Diabetes Co-Existing with Myocardial Infarction
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Myocardial Salvaging Effects of Berberine in Experimental Diabetes Co-Existing with Myocardial Infarction

机译:小ber碱对实验性糖尿病与心肌梗死并存的心肌的挽救作用

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Introduction: Berberine, an isoquinoline alkaloid isolated from the Berberis aristata, has been shown to display a wide array of pharmacological activities (hypoglycaemic and hypolipidemic). Aim: The present study was designed to investigate whether these pharmacological properties translate into the cardioprotective effects of Berberine in the setting of diabetes mellitus. Materials and Methods: Necessary approval from the Institutional Animal Ethics Committee was taken for the study. Experimental diabetes was produced with single dose of Streptozotocin (STZ): 45mg/kg ip and myocardial infarction was induced by administering Isoproterenol (ISP): 85mg/kg, sc to rats on 35th & 36th day. After the confirmation of diabetes on 7th day (>200mg/dl), Berberine (100 mg/kg) was administered orally to experimental rats from day 8 and continued for 30 days thereafter. Various anti-diabetic (Glucose, HbA1c), cardioprotective (CPK-MB), metabolic (lipid profile), safety {liver function (SGPT, kidney function (Creatinine)} and histopathological indices of injury were evaluated in Healthy Control, Diabetic Control and Berberine treated groups. Results: Administration of STZ-ISP resulted in a significant decrease in body weight (p<0.001), diabetic changes (increase in blood glucose, HbA1c), cardiac injury (leakage of myocardial CPK-MB), altered lipid profile, SGPT, creatinine levels (p<0.001) in the diabetic control group rats as compared to healthy control. Berberine treatment demonstrated significant antidiabetic as well as myocardial salvaging effects as indicated by restoration of blood glucose, HbA1c and CPK-MB levels (p<0.001) compared to diabetic control group. In addition, Berberine favourably modulated the lipid parameters (total cholesterol, triglycerides, HDL, LDL). Subsequent to ISP challenge, histopathological assessment of heart, pancreas and biochemical indices of injury confirmed the cardioprotective effects of Berberine in setting of diabetes. In addition, Berberine was found to be safe to the liver and kidney. Conclusion: Berberine treatment produced myocardial salvaging effects in the setting of diabetes challenged with ISP induced myocardial necrosis. Cardioprotection may be attributed to anti-diabetic and hypolipidemic activities.
机译:简介:小ber碱是一种从小Ber小isolated中分离的异喹啉生物碱,已显示出多种药理活性(降血糖和降血脂)。目的:本研究旨在研究这些药理特性在糖尿病情况下是否转化为小ber碱的心脏保护作用。材料和方法:进行了研究,并获得了机构动物伦理委员会的批准。用单剂量链脲佐菌素(STZ):45mg / kg ip产生实验性糖尿病,并在第35天和第36天对大鼠施用异丙肾上腺素(ISP):85mg / kg,皮下注射诱导心肌梗塞。在第7天确认糖尿病(> 200mg / dl)后,从第8天开始对实验大鼠口服黄连素(100 mg / kg),此后持续30天。在健康对照,糖尿病对照和糖尿病对照中评估了各种抗糖尿病药(葡萄糖,HbA1c),心脏保护药(CPK-MB),代谢(脂质谱),安全性{肝功能(SGPT,肾功能(肌酐)}}和组织病理学指标。小碱治疗组结果:STZ-ISP的使用导致体重(p <0.001),糖尿病变化(血糖,HbA1c升高),心脏损伤(心肌CPK-MB泄漏)显着降低。与健康对照组相比,糖尿病对照组大鼠的SGPT,肌酐水平(p <0.001)。小。碱治疗具有显着的抗糖尿病和心肌挽救作用,如血糖,HbA1c和CPK-MB水平的恢复(p <与糖尿病对照组相比为0.001),此外,小ine碱可很好地调节脂质参数(总胆固醇,甘油三酸酯,HDL,LDL),随后ISP攻击,心脏,胰腺和肝脏的组织病理学评估d损伤的生化指标证实了黄连素对糖尿病的保护作用。此外,发现小Ber碱对肝脏和肾脏安全。结论:小ber碱治疗在ISP引起的心肌坏死所致的糖尿病中具有心肌挽救作用。心脏保护作用可能归因于抗糖尿病和降血脂活性。

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