Urolithin A promotes p62-dependent lysophagy to prevent acute retinal neurodegeneration.

IF 14.9 1区 医学 Q1 NEUROSCIENCES
Juan Ignacio Jiménez-Loygorri, Álvaro Viedma-Poyatos, Raquel Gómez-Sintes, Patricia Boya
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引用次数: 0

Abstract

Background: Age-related macular degeneration (AMD) is the leading cause of blindness in elderly people in the developed world, and the number of people affected is expected to almost double by 2040. The retina presents one of the highest metabolic demands in our bodies that is partially or fully fulfilled by mitochondria in the neuroretina and retinal pigment epithelium (RPE), respectively. Together with its post-mitotic status and constant photooxidative damage from incoming light, the retina requires a tightly-regulated housekeeping system that involves autophagy. The natural polyphenol Urolithin A (UA) has shown neuroprotective benefits in several models of aging and age-associated disorders, mostly attributed to its ability to induce mitophagy and mitochondrial biogenesis. Sodium iodate (SI) administration recapitulates the late stages of AMD, including geographic atrophy and photoreceptor cell death.

Methods: A combination of in vitro, ex vivo and in vivo models were used to test the neuroprotective potential of UA in the SI model. Functional assays (OCT, ERGs), cellular analysis (flow cytometry, qPCR) and fine confocal microscopy (immunohistochemistry, tandem selective autophagy reporters) helped address this question.

Results: UA alleviated neurodegeneration and preserved visual function in SI-treated mice. Simultaneously, we observed severe proteostasis defects upon SI damage induction, including autophagosome accumulation, that were resolved in animals that received UA. Treatment with UA restored autophagic flux and triggered PINK1/Parkin-dependent mitophagy, as previously reported in the literature. Autophagy blockage caused by SI was caused by severe lysosomal membrane permeabilization. While UA did not induce lysosomal biogenesis, it did restore upcycling of permeabilized lysosomes through lysophagy. Knockdown of the lysophagy adaptor SQSTM1/p62 abrogated viability rescue by UA in SI-treated cells, exacerbated lysosomal defects and inhibited lysophagy.

Conclusions: Collectively, these data highlight a novel putative application of UA in the treatment of AMD whereby it bypasses lysosomal defects by promoting p62-dependent lysophagy to sustain proteostasis.

尿囊素 A 可促进 p62 依赖性溶血作用,防止急性视网膜神经变性。
背景:老年性黄斑变性(AMD)是发达国家老年人失明的主要原因,预计到 2040 年,患病人数将增加近一倍。视网膜是人体新陈代谢需求最高的部位之一,而神经视网膜和视网膜色素上皮(RPE)中的线粒体分别部分或完全满足了视网膜的新陈代谢需求。由于视网膜处于后有丝分裂状态,并不断受到入射光的光氧化损伤,因此需要一个严格调控的自噬内务系统。天然多酚乌洛托品 A(UA)已在多种衰老和年龄相关疾病模型中显示出神经保护作用,这主要归因于其诱导有丝分裂和线粒体生物生成的能力。碘酸钠(SI)能再现老年性视网膜病变的晚期阶段,包括地理萎缩和感光细胞死亡:方法:结合体外、体外和体内模型,测试 UA 在 SI 模型中的神经保护潜力。功能测试(OCT、ERGs)、细胞分析(流式细胞术、qPCR)和精细共聚焦显微镜(免疫组化、串联选择性自噬报告)有助于解决这一问题:结果:尿崩症缓解了 SI 治疗小鼠的神经退行性变,并保护了其视觉功能。同时,我们观察到在诱导 SI 损伤时出现了严重的蛋白稳态缺陷,包括自噬体积累,而接受 UA 治疗的动物则解决了这一问题。正如之前文献报道的那样,用 UA 治疗可恢复自噬通量并触发 PINK1/Parkin 依赖性有丝分裂。SI导致的自噬阻断是由严重的溶酶体膜通透性引起的。虽然 UA 不能诱导溶酶体的生物生成,但它确实通过溶酶吞噬恢复了通透溶酶体的上行循环。溶酶体吞噬适配体 SQSTM1/p62 的敲除削弱了 UA 对 SI 处理细胞的存活率的挽救作用,加剧了溶酶体缺陷并抑制了溶酶体吞噬:总之,这些数据强调了 UA 在治疗 AMD 中的一种新的可能应用,即通过促进 p62 依赖性溶酶体吞噬来维持蛋白稳态,从而绕过溶酶体缺陷。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Molecular Neurodegeneration
Molecular Neurodegeneration 医学-神经科学
CiteScore
23.00
自引率
4.60%
发文量
78
审稿时长
6-12 weeks
期刊介绍: Molecular Neurodegeneration, an open-access, peer-reviewed journal, comprehensively covers neurodegeneration research at the molecular and cellular levels. Neurodegenerative diseases, such as Alzheimer's, Parkinson's, Huntington's, and prion diseases, fall under its purview. These disorders, often linked to advanced aging and characterized by varying degrees of dementia, pose a significant public health concern with the growing aging population. Recent strides in understanding the molecular and cellular mechanisms of these neurodegenerative disorders offer valuable insights into their pathogenesis.
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