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首页> 外文期刊>Journal of Pharmacy and Pharmacology >Protective effects of benidipine on hydrogen peroxide-induced injury in rat isolated hearts.
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Protective effects of benidipine on hydrogen peroxide-induced injury in rat isolated hearts.

机译:贝尼地平对离体心脏中过氧化氢诱导的损伤的保护作用。

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We investigated the effects of benidipine (hydrochloride), a calcium antagonist, on hydrogen peroxide (H(2)O(2))-induced injury in Langendorff-perfused rat hearts. The hearts were aerobically perfused at a constant flow and exposed to H(2)O(2) (600 micromol L(-1)) for 4 min, resulting in the oxidative stress-induced myocardial dysfunction (e.g., decrease in the left ventricular developed pressure) and myocardial cell injury (e.g., increase in the release of lactate dehydrogenase). Pretreatment of the hearts with benidipine or nifedipine was performed for 20 min until the start of H(2)O(2) exposure. Benidipine at 1 nmol L(-1) and nifedipine at 10 nmol L(-1) decreased the myocardial contractility and perfusion pressure to a similar degree in the hearts under normal conditions. Benidipine (1 nmol L(-1)) significantly reduced the H(2)O(2)-induced myocardial damage. Nifedipine (10 nmol L(-1)) also tended to exhibit similar effects. Benidipine inhibited the increase in tissue lipid peroxidation induced by H(2)O(2). The results suggest that, in addition to the calcium antagonism, benidipine possesses other actions responsible for the cardioprotective effects, to which the antioxidant activity of benidipine may partly contribute.
机译:我们调查了贝尼地平(盐酸盐),一种钙拮抗剂,对过氧化氢(H(2)O(2))诱导的Langendorff灌注大鼠心脏损伤的影响。心脏以恒定流量进行有氧灌注,并暴露于H(2)O(2)(600 micromol L(-1))4分钟,导致氧化应激诱导的心肌功能障碍(例如,左心室减少)压力升高)和心肌细胞损伤(例如乳酸脱氢酶释放增加)。用贝尼地平或硝苯地平对心脏进行预处理20分钟,直到H(2)O(2)暴露开始。在正常条件下,心脏的Benidipine在1 nmol L(-1)和硝苯地平在10 nmol L(-1)降低心肌收缩力和灌注压力。贝尼地平(1 nmol L(-1))大大减少H(2)O(2)诱导的心肌损害。硝苯地平(10 nmol L(-1))也倾向于表现出相似的作用。贝尼地平抑制H(2)O(2)诱导的组织脂质过氧化的增加。结果表明,除了钙拮抗作用外,贝尼地平还具有其他作用于心脏的保护作用,贝尼地平的抗氧化活性可能对此部分起作用。

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