Nrf2 -血红素加氧酶途径可能参与非瑟酮抗白内障活性的药理研究

Krishna Reddy BV, Avinash Kumar Reddy G, Sujitha V, Manasa A
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引用次数: 1

摘要

糖尿病或糖尿病现在是一种流行病,患者人口的百分比上升到世界人口的近10%。在所有糖尿病并发症中,白内障导致约60%的糖尿病患者致残。但糖尿病性白内障的发病机制仍是医学上的一个不完全了解的领域,给治疗带来了难题。我们目前掌握的数据足以证明氧化应激在DM并发症如DM肾病、DM神经病变、心脏肥厚等的发病机制中起主要作用,提示氧化应激是糖尿病的核心特征。本研究对非塞汀基于糖尿病的抗白内障特性进行药理学评价。本研究集中于估计Nrf-2 /血红素加氧酶(HO)途径可能参与观察到的治疗效果,如果有的话。本研究获得的数据也表明,观察到的有益作用主要是由于Nrf2/HO-1通路的激活。这些作用可能导致组织抗氧化状态的增加以及自由基产生的减少,这最终导致了观察到的非西汀对高血糖性白内障的有益作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pharmacological study on the possible involvement of a Nrf2 -Heme oxygenase pathways in anti-cataract activity of fisetin
DM otherwise diabetes is now a days an epidemic with the percentage of patient population rising to almost 10% of the world population. Out of all the DM complications, cataract leads the way contributing to disabilities to about 60% of diabetic population. But the pathogenesis of DM cataract is still a half-understood area of medicine there by posing a problem in the therapy. The data that we have till now gives us enough evidence to advocate the oxidative stress has a major role for the pathogenesis of DM complications like DMnephropathy, DMneuropathy, and cardiac hypertrophy, which suggests the oxidative stress is a central feature of diabetes. In the current research, the pharmacological evaluation of Fisetin for its DM based anti-cataract property was performed. This research concentrates to estimate the possible involvement of Nrf-2 / heme oxygenase (HO)-pathway in the observed therapeutic effect, if any. The data obtained in this study also indicate that the observed beneficial effects mainly due to activation of Nrf2/HO-1 pathway. These effects probably result in increased tissue anti-oxidant status as well as decreased free radical production, which ultimately responsible for the observed beneficial effects of Fisetin against hyperglycemia-induced cataract.
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