一个假设MiRNA-124 介导的 sirtuin 1 和维生素 D 受体基因表达调控会加速衰老

IF 2.2 Q3 GERIATRICS & GERONTOLOGY
Aging Medicine Pub Date : 2024-06-15 DOI:10.1002/agm2.12330
Poulami Dhar, Shailaja Moodithaya, Prakash Patil, Kellarai Adithi
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引用次数: 0

摘要

随着年龄的增长、生活方式和环境的变化,特定的 miRNA 显然会过度表达。先前的研究报告了 miR-124 在老化皮肤、老年性认知障碍、缺血性心脏病、肌肉萎缩和骨折等不同情况下的过表达。因此,miR-124 被认为是建立衰老表观基因组假说的可靠 miRNA 靶点。同时,该假说还把 SIRT1 和 VDR 基因的表达作为这一特定 miRNA 表达的靶点,因为这些基因被认为与衰老有关。本研究旨在从过去有关衰老的研究中得出事实和证据。我们在 TargetScan 和 miRbase 数据库中进行了硅学搜索,以分析与衰老相关的 miRNA 及其基因靶标,并使用 Python seaborn 文库,以柱状图的形式表示结果。和 miR-124-3p.2 以 VDR 和 SIRT1 基因的 3′ UTR 为靶标,从而表明 miR-124 可调控这些基因的表达。此外,少数体外研究观察到,miR-124 过表达会导致 VDR 和 SIRT1 基因表达下调。总之,本研究推测,miR-124 的过度表达会降低 VDR 和 SIRT1 基因的表达,从而推进衰老进程,导致老年相关并发症的发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A hypothesis: MiRNA-124 mediated regulation of sirtuin 1 and vitamin D receptor gene expression accelerates aging

A hypothesis: MiRNA-124 mediated regulation of sirtuin 1 and vitamin D receptor gene expression accelerates aging

Objectives

Specific miRNAs are evident to be overexpressed with age, lifestyle, and environmental changes. Previous studies reported miR-124 overexpression in different scenarios in aged skin, age-related cognitive impairment, ischemic heart disease, muscle atrophy, and fractures. Thus miR-124 was considered to be a reliable miRNA target to establish a hypothesis on aging epigenome. Parallelly the hypothesis focuses on the expression of SIRT1 and VDR genes as a target for this specific miRNA expression as these genes were believed to be related to aging. This study aims to derive facts and evidence from past studies on aging. The objective was to establish a hypothetical linkage between miR-124 with age-related genes like SIRT1 and VDR.

Methods

An in silico search was performed in the TargetScan and miRbase databases to analyze the aging-associated miRNAs and their gene targets, the Python seaborn library was used, and the results were represented in terms of a bar plot.

Results

Based on an in silico analysis and studies available in the literature, we identified that miR-124-3p.1 and miR-124-3p.2 targets 3′ UTR of VDR and SIRT1 genes, and hence thereby indicates that the miR-124 can regulate the expression of these genes. Further, few in vitro research studies have observed that miR-124 overexpression leads to the downregulation of VDR and SIRT1 gene expression. These results indicate that the suppression of these target genes accelerates early aging and age-related disorders.

Conclusions

Overall, this study hypothesizes that the overexpression of miR-124 diminishes the expression of VDR and SIRT1 genes, and thereby advances the process of aging, resulting in the development of age-associated complications.

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来源期刊
Aging Medicine
Aging Medicine Medicine-Geriatrics and Gerontology
CiteScore
4.10
自引率
0.00%
发文量
38
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