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局部给予 ACE 抑制剂可中断两肾一夹型高血压性白内障模型中白内障的进展。

Topical Administration of ACE Inhibitor Interrupts the Progression of Cataract in Two Kidney One Clip Induced Hypertensive Cataract Model.

机构信息

Department of Pharmacology, Institute of Pharmaceutical Sciences, Guru Ghasidas Vishwavidyalaya (A Central University), Koni, Bilaspur, India.

Department of Pharmacology, Rungta Institute of Pharmaceutical Sciences and Research, Rungta Group of Colleges, Bhilai, India.

出版信息

Curr Eye Res. 2022 Mar;47(3):399-408. doi: 10.1080/02713683.2021.2002911. Epub 2021 Nov 12.

Abstract

PURPOSE

Previously, we assessed that hypertension increases cataractogenesis. In the present study, we evaluated the effect of oral and topical administration of enalapril on two kidney one clip (2K1C)-induced hypertensive cataract model by evaluating the biochemical alteration of lenticular antioxidants, ionic content, ATPase activity, protein content and careful examination of the lenticular opacity.

MATERIALS AND METHOD

Animals were divided into normal and hypertensive animals. Hypertensive animals were divided into hypertensive control group (0.3% CMC), enalapril (oral) treatment group (20 mg/kg/day; p.o), and enalapril (topical) treatment group (0.1% w/v on the eye cornea) for a period of twelve weeks. During experimental study blood pressure, heart rate and morphology of the eyes were monitored biweekly. After twelve weeks, lenses were photographed and various catractogenic biochemical parameters were assessed.

RESULTS

Enalapril (oral) treatment conserved the blood pressure (systolic and diastolic), restored the level of antioxidants, restored the lipid peroxidation marker, nitrite content, ionic content, ATPase function, protein content, and thus delayed the cataract formation. While, enalapril (topical) treatment exhibited anti-cataract effect without affecting the systolic and diastolic blood pressure that could be by restoring the antioxidant level, maintaining the ionic balance, balancing the protein levels, and by inhibiting the upregulated ocular renin angiotensin system. The overall results suggest that enalapril (topical) treatment showed conspicuous effect than enalapril (oral) treatment in adjourning the cataract formation.

CONCLUSION

Based on the results, it may be concluded that upregulated ocular RAS by increasing oxidative stress and by misbalancing the lenticular ionic and protein content may lead to cataract formation in hypertensive condition.

摘要

目的

此前,我们评估了高血压会增加白内障的形成。在本研究中,我们通过评估晶状体抗氧化剂的生化改变、离子含量、ATP 酶活性、蛋白质含量以及对晶状体混浊的仔细检查,评估了口服和局部给予依那普利对两肾一夹(2K1C)诱导的高血压性白内障模型的影响。

材料和方法

动物分为正常和高血压动物。高血压动物分为高血压对照组(0.3%CMC)、依那普利(口服)治疗组(20mg/kg/天;po)和依那普利(局部)治疗组(眼角膜 0.1%w/v),为期 12 周。在实验研究中,每两周监测一次血压、心率和眼部形态。12 周后,对晶状体进行拍照,并评估各种白内障形成的生化参数。

结果

依那普利(口服)治疗可维持血压(收缩压和舒张压),恢复抗氧化剂水平,恢复脂质过氧化标志物、亚硝酸盐含量、离子含量、ATP 酶功能、蛋白质含量,从而延缓白内障的形成。而依那普利(局部)治疗在不影响收缩压和舒张压的情况下表现出抗白内障作用,这可能是通过恢复抗氧化剂水平、维持离子平衡、平衡蛋白质水平以及抑制上调的眼部肾素血管紧张素系统来实现的。总的结果表明,依那普利(局部)治疗在延缓白内障形成方面的效果比依那普利(口服)治疗更显著。

结论

基于这些结果,可以得出结论,上调的眼部 RAS 通过增加氧化应激和晶状体离子及蛋白质含量的失衡可能导致高血压状态下白内障的形成。

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