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miR-210 对于果蝇和小鼠的视网膜内稳态至关重要。

miR-210 is essential to retinal homeostasis in fruit flies and mice.

机构信息

Department of Biology, University of Padova, Padova, Italy.

Molecular Biotechnology Center (MBC) "Guido Tarone", Torino, Italy.

出版信息

Biol Direct. 2024 Oct 11;19(1):90. doi: 10.1186/s13062-024-00542-6.

Abstract

BACKGROUND

miR-210 is one of the most evolutionarily conserved microRNAs. It is known to be involved in several physiological and pathological processes, including response to hypoxia, angiogenesis, cardiovascular diseases and cancer. Recently, new roles of this microRNA are emerging in the context of eye and visual system homeostasis. Recent studies in Drosophila melanogaster unveiled that the absence of miR-210 leads to a progressive retinal degeneration characterized by the accumulation of lipid droplets and disruptions in lipid metabolism. However, the possible conservation of miR-210 knock-out effect in the mammalian retina has yet to be explored.

RESULTS

We further investigated lipid anabolism and catabolism in miR-210 knock-out (KO) flies, uncovering significant alterations in gene expression within these pathways. Additionally, we characterized the retinal morphology of flies overexpressing (OE) miR-210, which was not affected by the increased levels of the microRNA. For the first time, we also characterized the retinal morphology of miR-210 KO and OE mice. Similar to flies, miR-210 OE did not affect retinal homeostasis, whereas miR-210 KO mice exhibited photoreceptor degeneration. To explore other potential parallels between miR-210 KO models in flies and mice, we examined lipid metabolism, circadian behaviour, and retinal transcriptome in mice, but found no similarities. Specifically, RNA-seq confirmed the lack of involvement of lipid metabolism in the mice's pathological phenotype, revealing that the differentially expressed genes were predominantly associated with chloride channel activity and extracellular matrix homeostasis. Simultaneously, transcriptome analysis of miR-210 KO fly brains indicated that the observed alterations extend beyond the eye and may be linked to neuronal deficiencies in signal detection and transduction.

CONCLUSIONS

We provide the first morphological characterization of the retina of miR-210 KO and OE mice, investigating the role of this microRNA in mammalian retinal physiology and exploring potential parallels with phenotypes observed in fly models. Although the lack of similarities in lipid metabolism, circadian behaviour, and retinal transcriptome in mice suggests divergent mechanisms of retinal degeneration between the two species, transcriptome analysis of miR-210 KO fly brains indicates the potential existence of a shared upstream mechanism contributing to retinal degeneration in both flies and mammals.

摘要

背景

miR-210 是最具进化保守性的 microRNA 之一。已知它参与多种生理和病理过程,包括对缺氧的反应、血管生成、心血管疾病和癌症。最近,这种 microRNA 的新作用在眼睛和视觉系统稳态的背景下出现。最近在黑腹果蝇中的研究表明,miR-210 的缺失导致进行性视网膜变性,其特征是脂质滴的积累和脂质代谢的破坏。然而,miR-210 敲除效应在哺乳动物视网膜中的可能保守性尚未得到探索。

结果

我们进一步研究了 miR-210 敲除 (KO) 果蝇中的脂质合成和分解代谢,揭示了这些途径中基因表达的显著改变。此外,我们描述了过表达 (OE) miR-210 的果蝇的视网膜形态,发现microRNA 水平的增加对其没有影响。我们首次还描述了 miR-210 KO 和 OE 小鼠的视网膜形态。与果蝇类似,miR-210 OE 不影响视网膜内稳态,而 miR-210 KO 小鼠则表现出光感受器变性。为了探索果蝇和小鼠中 miR-210 KO 模型之间的其他潜在相似性,我们检查了小鼠中的脂质代谢、昼夜节律行为和视网膜转录组,但未发现相似性。具体而言,RNA-seq 证实脂质代谢不参与小鼠的病理表型,表明差异表达的基因主要与氯通道活性和细胞外基质稳态有关。同时,miR-210 KO 果蝇大脑的转录组分析表明,观察到的改变不仅限于眼睛,并且可能与信号检测和转导中的神经元缺陷有关。

结论

我们提供了 miR-210 KO 和 OE 小鼠视网膜的首次形态学描述,研究了该 microRNA 在哺乳动物视网膜生理学中的作用,并探索了与果蝇模型中观察到的表型之间的潜在相似性。尽管在小鼠中脂质代谢、昼夜节律行为和视网膜转录组中缺乏相似性表明两种物种的视网膜变性机制不同,但 miR-210 KO 果蝇大脑的转录组分析表明,可能存在一个共同的上游机制导致果蝇和哺乳动物的视网膜变性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6cfb/11468086/0826e05af8c4/13062_2024_542_Fig1_HTML.jpg

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