首页> 外文期刊>The Journal of biological chemistry >Pretreatment with Pyridoxamine Mitigates Isolevuglandin-associated Retinal Effects in Mice Exposed to Bright Light
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Pretreatment with Pyridoxamine Mitigates Isolevuglandin-associated Retinal Effects in Mice Exposed to Bright Light

机译:用吡哆胺的预处理减轻了暴露于明亮光的小鼠中的isolevglandin相关的视网膜效应

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The benefits of antioxidant therapy for treating age-related macular degeneration, a devastating retinal disease, are limited. Perhaps species other than reactive oxygen intermediates should be considered as therapeutic targets. These could be lipid peroxidation products, including isolevuglandins (isoLGs), prototypical and extraordinarily reactive γ-ketoaldehydes that avidly bind to proteins, phospholipids, and DNA and modulate the properties of these biomolecules. We found isoLG adducts in aged human retina but not in the retina of mice kept under dim lighting. Hence, to test whether scavenging of isoLGs could complement or supplant antioxidant therapy, we exposed mice to bright light and found that this insult leads to retinal isoLG-adduct formation. We then pretreated mice with pyridoxamine, a B6 vitamer and efficient scavenger of γ-ketoaldehydes, and found that the levels of retinal isoLG adducts are decreased, and morphological changes in photoreceptor mitochondria are not as pronounced as in untreated animals. Our study demonstrates that preventing the damage to biomolecules by lipid peroxidation products, a novel concept in vision research, is a viable strategy to combat oxidative stress in the retina.
机译:抗氧化治疗治疗年龄相关性黄斑变性,毁灭性视网膜疾病的益处有限。可能除了反应性氧中间体以外的物种应被视为治疗靶标。这些可以是脂质过氧化产物,包括isolevuglandins(Ismols),原型和非凡的反应性γ-酮醛,其蚕晶,磷脂和DNA与蛋白质,磷脂和DNA常用,并调节这些生物分子的性质。我们发现在老年人视网膜中的ISOLG加合物,但不在小鼠的视网膜中保持在昏暗的灯光下。因此,为了测试孤立性是否可以补充或取代抗氧化治疗,我们将小鼠暴露于明亮的光线,发现这种侮辱导致视网膜ISOLG加合物形成。然后用吡哆胺进行预处理小鼠,B6维生素和γ-酮醛的有效清除剂,发现视网膜ISOLG加合物的水平降低,并且感光体线粒体的形态变化并不像未处理的动物那样明显。我们的研究表明,防止脂质过氧化产品的损伤,这是视觉研究的新概念,是对抗视网膜氧化应激的可行策略。

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