Maher Pamela, Hanneken Anne
Department of Cell Biology, The Scripps Research Institute, La Jolla, CA, USA.
Invest Ophthalmol Vis Sci. 2005 Feb;46(2):749-57. doi: 10.1167/iovs.04-0883.
PURPOSE: To characterize the molecular basis of oxidative stress-induced death, a process that has been implicated in several chronic eye diseases, in RGC-5 cells, an immortalized retinal ganglion cell (RGC) line. METHODS: The responses of RGC-5 cells to oxidative stress induced by three different treatments--glutathione depletion, tert-butyl peroxide addition, and hydrogen peroxide addition--were examined and compared. The level of cell death was monitored with the MTT assay. The effects of glutathione depletion on the intracellular levels of glutathione, reactive oxygen species, and calcium were determined. The type of cell death was assessed with assays for DNA fragmentation and caspase activation. Compounds that were shown to be protective of central nervous system-derived nerve cells exposed to oxidative stress were tested to see whether they could also protect the RGC-5 cells. In addition, several compounds that have been found to be protective in primary cultures of RGCs or in animal models of retinal dysfunction were tested against each of the inducers of oxidative stress. RESULTS: The cell death triggered by all three inducers of oxidative stress shared several features, suggesting that there is a final common pathway of oxidative stress-induced death in the RGCs. In addition, several compounds were identified that protected RGCs from multiple forms of oxidative stress. CONCLUSIONS: The RGC-5 line is an excellent model for studying mechanisms of RGC death in response to oxidative stress and for the identification of neuroprotective compounds.
目的:在永生视网膜神经节细胞(RGC)系RGC-5细胞中,明确氧化应激诱导性死亡的分子基础,这一过程与多种慢性眼部疾病有关。 方法:检测并比较RGC-5细胞对三种不同处理(谷胱甘肽耗竭、添加叔丁基过氧化氢和添加过氧化氢)诱导的氧化应激的反应。用MTT法监测细胞死亡水平。测定谷胱甘肽耗竭对细胞内谷胱甘肽、活性氧和钙水平的影响。通过DNA片段化检测和半胱天冬酶激活检测评估细胞死亡类型。测试已证明对暴露于氧化应激的中枢神经系统来源神经细胞有保护作用的化合物,看它们是否也能保护RGC-5细胞。此外,测试几种已发现对RGC原代培养物或视网膜功能障碍动物模型有保护作用的化合物,以对抗每种氧化应激诱导剂。 结果:由所有三种氧化应激诱导剂引发的细胞死亡具有几个共同特征,表明RGC中存在氧化应激诱导性死亡的最终共同途径。此外,鉴定出几种能保护RGC免受多种形式氧化应激的化合物。 结论:RGC-5细胞系是研究RGC对氧化应激反应中细胞死亡机制以及鉴定神经保护化合物的优秀模型。
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