The protective effects of aspirin on the α-crystalline molecular chaperone-like activity in naphthalene-induced cataract

Chinese Ophthalmic Research Pub Date : 2010-03-10 DOI:10.3969/J.ISSN.1003-0808.2010.03.009

Yan Chen, Yi Lu, Yongxiang Jiang, B. Qiu, Jie Tian

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引用次数: 1

Abstract

Background Age-related cataract is the leading cause of visual impairment worldwide.To seek the effective prevention and drugs for management of cataract is important.Naphthalene-induced cataract of rat is an ideal animal model for the research of human age-related cataract,and aspirin has been proven to inhibit the development of human age-related cataract.ObjectiveThe present study is to investigate the role of aspirin on naphthalene-induced cataract.Methods Forty-five 150-160 g female SD rats were divided into three groups randomly.Naphthalene was orally taken with 0.5mg/kg per day for 3 days and then 1mg/kg per day for 70 days,and then 100mg/kg of aspirin was given per day for 70 days following four-day washout period in group A.In group B,the animals was given orally only naphthalene at the same way.No any intervention was used in group C.Naphthalene-induced cataract was examined under the slim lamp every week.The experimental animals were sacrificed and lenses were obtained in 70 days.α-Crystalline was extracted from lens homogenate and purified and identified using High Performance Liquid Chromatography(HPLC),2-dimentional electrophoresis gel and Western blot.Different abilities of α-crystalline to protect β low crystalline from aggregation were observed using ultraviolet spectrophotometer.Results Naphthalene-induced cataract formed at the third week in only naphthalene group but at the sixth week in naphthalene+aspirin group under the slim lamp.No significant difference was found in the degree of lenses opacity in the second week among these three groups(F=0.032,P=0.969).However,a statistically significant difference was seen in the degree of lenses opacity in the fourth,sixth,eighth and tenth week among these three groups(F= 5031.130,P=0.000;F=115964.000,P=0.000;F=169846.500,P=0.000;F= 195431.200,P=0.000).Themolecular chaperone-like activity was significantly higher than that of the naphthalene-induced group.Conclusion Aspirin delays the progression of lens opacification through protecting α-crystalline molecular chaperone-like activity. Key words: naphthalene-induced cataract; aspirin; α-crystalline; molecular chaperone-like activity

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阿司匹林对萘致白内障α-晶体分子伴侣样活性的保护作用

年龄相关性白内障是世界范围内视力损害的主要原因。寻求有效的预防和治疗白内障的药物是重要的。萘致大鼠白内障是研究人类老年性白内障的理想动物模型，阿司匹林已被证实对人类老年性白内障的发生有抑制作用。目的探讨阿司匹林在萘源性白内障中的作用。方法150 ~ 160 g雌性SD大鼠45只，随机分为3组。a组小鼠每天口服萘0.5mg/kg，连续3天，然后每天口服1mg/kg，连续70天，4天洗脱期后，每天口服阿司匹林100mg/kg，连续70天。B组小鼠同样只口服萘。c组患者不采取任何干预措施，每周在薄灯下检查萘致白内障。70 d处死实验动物，获得晶状体。从晶状体匀浆中提取α-晶体，采用高效液相色谱(HPLC)、二维电泳凝胶和Western blot对α-晶体进行纯化和鉴定。用紫外分光光度计观察了α-晶体对β低晶聚集的不同保护能力。结果单用萘组在第3周形成萘致白内障，萘+阿司匹林组在第6周形成。两组患者术后第2周晶状体混浊程度比较，差异无统计学意义(F=0.032,P=0.969)。但三组在术后第4、6、8、10周的晶状体混浊程度差异有统计学意义(F= 5031.130,P=0.000;F=115964.000,P=0.000;F=169846.500,P=0.000;F= 195431.200,P=0.000)。分子伴侣样活性明显高于萘诱导组。结论阿司匹林通过保护α-晶体分子伴侣样活性延缓晶状体混浊的进展。关键词:萘致白内障;阿斯匹林;α晶;分子伴侣样活性

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Chinese Ophthalmic Research

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