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小鼠骨骼肌和脂肪组织中的可变剪接图谱:间歇性禁食和运动的影响。

Alternative splicing landscape in mouse skeletal muscle and adipose tissue: Effects of intermittent fasting and exercise.

作者信息

Gaugel Jasmin, Jähnert Markus, Neumann Alexander, Heyd Florian, Schürmann Annette, Vogel Heike

机构信息

Research Group Nutrigenomics of Obesity and Department of Experimental Diabetology, German Institute of Human Nutrition Potsdam-Rehbruecke, Nuthetal, Germany; German Center for Diabetes Research (DZD), München-Neuherberg, Germany; Research Group Molecular and Clinical Life Science of Metabolic Diseases, Faculty of Health Sciences Brandenburg, University of Potsdam, Brandenburg, Germany.

Research Group Nutrigenomics of Obesity and Department of Experimental Diabetology, German Institute of Human Nutrition Potsdam-Rehbruecke, Nuthetal, Germany; German Center for Diabetes Research (DZD), München-Neuherberg, Germany.

出版信息

J Nutr Biochem. 2025 Mar;137:109837. doi: 10.1016/j.jnutbio.2024.109837. Epub 2024 Dec 25.

Abstract

Alternative splicing contributes to diversify the cellular protein landscape, but aberrant splicing is implicated in many diseases. To which extent mis-splicing contributes to insulin resistance as the causal defect of type 2 diabetes and whether this can be reversed by lifestyle interventions is largely unknown. Therefore, RNA sequencing data from skeletal muscle and adipose tissue of diabetes-susceptible NZO mice treated with or without intermittent fasting and of healthy C57BL/6J mice subjected to exercise were analyzed for alternative splicing differences using Whippet and rMATS. Diet and exercise interventions triggered comparable levels of splicing changes, although the splicing profile of skeletal muscle appeared to be more flexible than that of adipose tissue, with 72-114 differential splicing events in muscle and less than 25 in adipose tissue. Splicing changes induced by time-restricted feeding, alternate-day fasting and exercise were generally mild, with a maximal percent spliced in (PSI) difference of 67%, indicating that alternative splicing plays a rather minor role in lifestyle-induced adaptations of muscle and adipose tissue in mice. However, intron retention contributed to the regulation of gene expression, influencing genes whose expression was directly linked to phenotypic parameters (e.g. Eno2 and Pan2). Alternate-day fasting promoted skipping of exon 7 in Mlxipl (coding for ChREBP), thereby affecting the glucose sensing module of this carbohydrate-responsive transcription factor. Both intermittent fasting and exercise training led to alternative splicing of known diabetes-related GWAS genes (e.g. Abcc8, Ifnar2, Smarcad1), highlighting the potential metabolic relevance of these changes.

摘要

可变剪接有助于使细胞蛋白质组多样化,但异常剪接与多种疾病有关。可变剪接在多大程度上作为2型糖尿病的因果缺陷导致胰岛素抵抗,以及这种情况是否可以通过生活方式干预得到逆转,目前尚不清楚。因此,使用Whippet和rMATS分析了糖尿病易感NZO小鼠在有或没有间歇性禁食情况下以及健康C57BL/6J小鼠运动后骨骼肌和脂肪组织的RNA测序数据,以寻找可变剪接差异。饮食和运动干预引发的剪接变化水平相当,尽管骨骼肌的剪接谱似乎比脂肪组织更灵活,肌肉中有72 - 114个差异剪接事件,脂肪组织中不到25个。限时喂养、隔日禁食和运动诱导的剪接变化通常较为轻微,最大剪接百分比差异(PSI)为67%,这表明可变剪接在小鼠生活方式诱导的肌肉和脂肪组织适应性变化中起的作用较小。然而,内含子保留参与了基因表达的调控,影响了那些其表达与表型参数直接相关的基因(如Eno2和Pan2)。隔日禁食促进了Mlxipl(编码ChREBP)中外显子7的跳跃,从而影响了这种碳水化合物反应性转录因子的葡萄糖感应模块。间歇性禁食和运动训练都导致了已知的与糖尿病相关的全基因组关联研究(GWAS)基因的可变剪接(如Abcc8、Ifnar2、Smarcad1),突出了这些变化潜在的代谢相关性。

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