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miR-486 对于肌肉功能至关重要,并能抑制肌营养不良转录组。

miR-486 is essential for muscle function and suppresses a dystrophic transcriptome.

机构信息

Department of Pediatrics, Division of Neurology at Children's of Alabama and the University of Alabama at Birmingham, Birmingham, AL, USA.

University of Alabama at Birmingham Center for Exercise Medicine (UCEM), Birmingham, AL, USA.

出版信息

Life Sci Alliance. 2022 May 5;5(9). doi: 10.26508/lsa.202101215. Print 2022 Sep.

Abstract

miR-486 is a muscle-enriched microRNA, or "myomiR," that has reduced expression correlated with Duchenne muscular dystrophy (DMD). To determine the function of miR-486 in normal and dystrophin-deficient muscles and elucidate miR-486 target transcripts in skeletal muscle, we characterized knockout mice ( KO). KO mice developed disrupted myofiber architecture, decreased myofiber size, decreased locomotor activity, increased cardiac fibrosis, and metabolic defects were exacerbated in KO: (DKO) mice. To identify direct in vivo miR-486 muscle target transcripts, we integrated RNA sequencing and chimeric miRNA eCLIP sequencing to identify key transcripts and pathways that contribute towards KO and dystrophic disease pathologies. These targets included known and novel muscle metabolic and dystrophic structural remodeling factors of muscle and skeletal muscle contractile transcript targets. Together, our studies identify miR-486 as essential for normal muscle function, a driver of pathological remodeling in dystrophin-deficient muscle, a useful biomarker for dystrophic disease progression, and highlight the use of multiple omic platforms to identify in vivo microRNA target transcripts.

摘要

miR-486 是一种富含肌肉的 microRNA,也称为“myomiR”,其表达水平降低与杜氏肌营养不良症(DMD)相关。为了确定 miR-486 在正常和肌营养不良蛋白缺陷肌肉中的功能,并阐明骨骼肌中的 miR-486 靶转录本,我们对 miR-486 敲除小鼠(KO)进行了表征。KO 小鼠表现出肌纤维结构紊乱、肌纤维大小减小、运动活性降低、心脏纤维化增加,并且在 KO:DKO 小鼠中代谢缺陷加剧。为了鉴定直接在体内的 miR-486 肌肉靶转录本,我们整合了 RNA 测序和嵌合 miRNA eCLIP 测序,以鉴定有助于 KO 和肌营养不良症病理的关键转录本和途径。这些靶标包括已知和新的肌肉代谢和肌营养不良症结构重塑因子,以及骨骼肌收缩转录本靶标。总之,我们的研究表明 miR-486 对于正常肌肉功能至关重要,是肌营养不良蛋白缺陷肌肉病理性重塑的驱动因素,是肌营养不良症进展的有用生物标志物,并强调了使用多种组学平台来鉴定体内 microRNA 靶转录本。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc83/9087951/28b2895a8886/LSA-2021-01215_GA.jpg

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