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The retinal pigment epithelium in Sorsby Fundus Dystrophy shows increased sensitivity to oxidative stress-induced degeneration

机译:Sorsby眼底营养不良症的视网膜色素上皮表现出对氧化应激诱导的变性的敏感性增加

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Sorsby Fundus Dystrophy (SFD) is a rare inherited autosomal dominant macular degeneration caused by specific mutations in TIMP3 . Patients with SFD present with pathophysiology similar to the more common Age-related Macular Degeneration (AMD) and loss of vision due to both choroidal neovascularization and geographic atrophy. Previously, it has been shown that RPE degeneration in AMD is due in part to oxidative stress. We hypothesized that similar mechanisms may be at play in SFD. The objective of this study was to evaluate whether mice carrying the S179C -Timp3 mutation, a variant commonly observed in SFD, showed increased sensitivity to oxidative stress. Antioxidant genes are increased at baseline in the RPE in SFD mouse models, but not in the retina. This suggests the presence of a pro-oxidant environment in the RPE in the presence of Timp3 mutations. To determine if the RPE of Timp3 mutant mice is more susceptible to degeneration when exposed to low levels of oxidative stress, mice were injected with low doses of sodium iodate. The RPE and photoreceptors in Timp3 mutant mice degenerated at low doses of sodium iodate, which had no effect in wildtype control mice. These studies suggest that TIMP3 mutations may result in a dysregulation of pro-oxidant—antioxidant homeostasis in the RPE, leading to RPE degeneration in SFD.
机译:Sorsby眼底营养不良(SFD)是由TIMP3的特异性突变引起的罕见遗传性常染色体显性黄斑变性。 SFD患者存在具有病理生理学的患者,类似于更常见的年龄相关的黄斑变性(AMD)和由于脉络膜新血管或地理萎缩而导致的视力丧失。以前,已经表明,AMD中的RPE变性部分是部分氧化应激。我们假设类似机制可能在SFD中发挥作用。本研究的目的是评估携带S179C -TIMP3突变的小鼠是否在SFD中常见的变体,表现出对氧化应激的敏感性增加。在SFD小鼠模型中的RPE中的基线下抗氧化基因增加,但不在视网膜中。这表明在存在TIMP3突变的情况下在RPE中存在促氧化环境。为了确定当暴露于低水平的氧化应激时更易于变性的TIMP3突变小鼠的RPE,用低剂量的碘酸钠注射小鼠。在低剂量的碘酸钠下退化的TIMP3突变小鼠中的RPE和光感受器在野生型对照小鼠中没有作用。这些研究表明,TiMp3突变可能导致RPE中促氧化剂 - 抗氧化剂稳定性的失调,导致SFD中的RPE变性。

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