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Profiling of circular RNAs in age-related cataract reveals circZNF292 as an antioxidant by sponging miR-23b-3p

机译:年龄相关性白内障的圆形RNA的分析揭示了Shonging MiR-23B-3P作为抗氧化剂的CirczNF292

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摘要

Age-related cataract (ARC) is one of the major causes of visual impairment and reversible blindness worldwide. Accumulating evidence has revealed that circular RNAs (circRNAs) are involved in multiple regulatory processes in various ocular diseases. However, the expression profile, regulatory roles, and underlying mechanisms of circRNAs in ARC remain largely unknown. Herein we deep-sequenced circRNAs of anterior lens capsules from normal and ARC lenses, and detected 23,787 candidate circRNAs. Of these, 466 were significantly differentially expressed, and a higher correlation in down-regulated circRNAs between ARC and diabetic cataract was observed compared with up-regulated ones. Subsequent bioinformatics analysis disclosed that certain differentially expressed circRNAs participated in oxidative stress and apoptosis-related signaling pathways in ARC. Notably, the level of circZNF292 was significantly decreased, while miR-23b-3p was significantly increased in ARC. The target region prediction and dual-luciferase reporter assays proved that circZNF292 acted as a competitive endogenous RNA to regulate the expression of anti-oxidative genes through competing with miR-23b-3p. Our results indicate that circZNF292, a down-regulated circRNA in the anterior lens capsule of ARC patients, may be involved in resistance to oxidative damage and apoptosis of lens epithelial cells by sponging miR-23b-3p, providing a potential target for prevention and treatment of ARC.
机译:与年龄相关的白内障(ARC)是全球视觉障碍和可逆失明的主要原因之一。积累证据表明,圆形RNA(Circrnas)参与了各种眼部疾病的多种调节过程。然而,弧中Circrnas的表达谱,调节作用和底层机制仍然很大程度上是未知的。在此,来自正常和弧镜头的前透镜胶囊的深序列芯片,并检测到23,787候选芯片。其中,466显着表达,与上调的相比,观察到弧形和糖尿病白内障之间的下调Circrnas的较高相关性。随后的生物信息学分析公开了某些差异表达的CircRNA参与弧形中的氧化应激和凋亡相关的信号传导途径。值得注意的是,CircZNF292的水平显着降低,而MiR-23B-3P在弧中显着增加。靶区域预测和双荧光素酶报告结果证明,CircZNF292作用为竞争内源性RNA,以通过竞争miR-23b-3p调节抗氧化基因的表达。我们的结果表明,弧形患者前镜头胶囊中的下调CircrNA,可能参与抗氧化损伤和透镜上皮细胞凋亡的抗性,通过海绵MiR-23b-3p,提供预防和治疗的潜在目标弧形。

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