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III类泛素结合酶在视网膜中的表达与分布

Expression and distribution of the class III ubiquitin-conjugating enzymes in the retina.

作者信息

Mirza Saima, Plafker Kendra S, Aston Christopher, Plafker Scott M

机构信息

Department of Cell Biology, University of Oklahoma Health Sciences Center, Oklahoma City, OK 73104, USA.

出版信息

Mol Vis. 2010 Nov 18;16:2425-37.

Abstract

PURPOSE

Mounting evidence implicates chronic oxidative stress as a significant pathogenic factor in the development and progression of retinopathies, including age-related macular degeneration (AMD). The age-dependent toxic accumulation of oxidatively damaged proteins, lipids, and DNA in susceptible cells of the retina arises, at least in part, from a decreased capacity to eliminate these damaged biomolecules. The goal of this study was to determine the expression patterns and function of class III ubiquitin-conjugating enzymes (UbcM3, UBE2E2, and UbcM2) in the retina. These enzymes have been implicated in the ubiquitin-dependent degradation of oxidatively damaged and misfolded proteins.

METHODS

Complementary western blotting and immunohistochemistry was performed with specific antibodies to determine the retinal cell expression pattern of each enzyme. Additional analyses using antibodies raised against UbcM2 were performed to determine the relative levels of the enzyme in lysates derived from various mouse organs as compared to the retina. An established light-damage model of oxidative stress-induced retinal degeneration was used to determine alterations in the susceptibility of mice harboring a single intact allele of UbcM2. Ubiquitin charging and auto-ubiquitylation assays were done to assess the catalytic state of UbcM2 following photo-oxidative stress.

RESULTS

Expression of the class III ubiquitin-conjugating enzymes in the retina, from highest to lowest, is UbcM2>UbcM3>UBE2E2. In addition to being the most robustly expressed, UbcM2 is further distinguished by its expression in photoreceptors and retinal pigment epithelial cells. UbcM2 is expressed in most mouse tissues analyzed and is most abundant in the retina. Studies using a bright-light-damage model of acute oxidative stress in mice harboring a single disrupted allele of UbcM2 revealed that a 58% reduction in enzyme levels did not increase the susceptibility of photoreceptors to acute photo-oxidative toxicity. This result may be explained by the observation that UbcM2 retained an intact and functional active site following exposure to acute bright light.

CONCLUSIONS

The class III ubiquitin-conjugating enzymes, and in particular UbcM2, are expressed in the retina and may function to counter the accumulation of oxidatively damaged and misfolded proteins. A 58% reduction in UbcM2 does not increase the susceptibility of photoreceptors to an acute photo-oxidative stress, suggesting the existence of compensating enzymes and/or that the remaining UbcM2 activity is sufficient to target oxidatively damaged proteins for destruction.

摘要

目的

越来越多的证据表明,慢性氧化应激是包括年龄相关性黄斑变性(AMD)在内的视网膜病变发生和发展的重要致病因素。视网膜易感细胞中氧化损伤的蛋白质、脂质和DNA随年龄增长而产生的毒性积累,至少部分源于清除这些受损生物分子的能力下降。本研究的目的是确定III类泛素结合酶(UbcM3、UBE2E2和UbcM2)在视网膜中的表达模式和功能。这些酶与氧化损伤和错误折叠蛋白质的泛素依赖性降解有关。

方法

使用特异性抗体进行蛋白质免疫印迹和免疫组织化学,以确定每种酶在视网膜细胞中的表达模式。使用针对UbcM2产生的抗体进行额外分析,以确定与视网膜相比,来自各种小鼠器官的裂解物中该酶的相对水平。利用已建立的氧化应激诱导视网膜变性的光损伤模型,确定携带单个完整UbcM2等位基因的小鼠易感性的变化。进行泛素充电和自泛素化测定,以评估光氧化应激后UbcM2的催化状态。

结果

III类泛素结合酶在视网膜中的表达,从高到低依次为UbcM2>UbcM3>UBE2E2。除了表达最为丰富外,UbcM2的独特之处还在于其在光感受器和视网膜色素上皮细胞中的表达。UbcM2在所分析的大多数小鼠组织中均有表达,且在视网膜中最为丰富。对携带单个UbcM2等位基因破坏的小鼠进行急性氧化应激强光损伤模型研究发现,酶水平降低58%并不会增加光感受器对急性光氧化毒性的易感性。这一结果可以通过以下观察结果来解释:UbcM2在暴露于急性强光后保留了完整且有功能的活性位点。

结论

III类泛素结合酶,尤其是UbcM2,在视网膜中表达,可能起到对抗氧化损伤和错误折叠蛋白质积累的作用。UbcM2降低58%并不会增加光感受器对急性光氧化应激的易感性,这表明存在补偿性酶和/或剩余的UbcM2活性足以将氧化损伤的蛋白质靶向降解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/092b/2994761/ea298ce920bb/mv-v16-2425-f1.jpg

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