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Mechanisms that minimize retinal impact of apolipoprotein E absence

机译:减少载脂蛋白E缺失对视网膜的影响的机制

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摘要

Apolipoprotein E (APOE) is a component of lipid-transporting particles and a recognition ligand for receptors, which bind these particles. The APOE isoform ε2 is a risk factor for age-related macular degeneration; nevertheless, APOE absence in humans and mice does not significantly affect the retina. We found that retinal cholesterol biosynthesis and the levels of retinal cholesterol were increased in mice, whereas cholesterol elimination by metabolism was decreased. No focal cholesterol deposits were observed in the retina. Retinal proteomics identified the most abundant cholesterol-related proteins in WT mice and revealed that, of these cholesterol-related proteins, only APOA4 had increased expression in the retina. In addition, there were changes in retinal abundance of proteins involved in proinflammatory and antiinflammatory responses, cellular cytoskeleton maintenance, vesicular traffic, and retinal iron homeostasis. The data obtained indicate that when APOE is absent, particles containing APOA1, APOA4, and APOJ still transport cholesterol in the intraretinal space, but these particles are not taken up by retinal cells. Therefore, cholesterol biosynthesis inside retinal cells increase, whereas metabolism to oxysterols decreases to prevent cells from cholesterol depletion. These and other compensatory changes underlie only a minor retinal phenotype in mice.
机译:载脂蛋白E(APOE)是脂质转运颗粒的组成部分,是结合这些颗粒的受体的识别配体。 APOE亚型ε2是与年龄相关的黄斑变性的危险因素;但是,人和小鼠中APOE的缺乏不会显着影响视网膜。我们发现,小鼠的视网膜胆固醇生物合成和视网膜胆固醇水平增加,而代谢消除胆固醇的程度降低。在视网膜中未观察到胆固醇沉积。视网膜蛋白质组学确定了WT小鼠中最丰富的胆固醇相关蛋白,并揭示了这些胆固醇相关蛋白中,只有APOA4在视网膜中表达增加。此外,视网膜中参与促炎和抗炎反应,细胞骨架维持,囊泡运输和视网膜铁稳态的蛋白质丰度也发生了变化。获得的数据表明,当缺少APOE时,含有APOA1,APOA4和APOJ的颗粒仍会在视网膜内空间转运胆固醇,但这些颗粒不会被视网膜细胞吸收。因此,视网膜细胞内部的胆固醇生物合成增加,而氧固醇的代谢减少,以防止细胞消耗胆固醇。这些和其他补偿性变化仅是小鼠视网膜视网膜表型的基础。

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