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超微结构免疫细胞化学显示老年小鼠骨骼肌核中 RNA 途径受损:与肌肉减少症有关?

Ultrastructural immunocytochemistry shows impairment of RNA pathways in skeletal muscle nuclei of old mice: A link to sarcopenia?

机构信息

Department of Neurosciences, Biomedicine and Movement Sciences, University of Verona.

出版信息

Eur J Histochem. 2021 Mar 24;65(2):3229. doi: 10.4081/ejh.2021.3229.

Abstract

During aging, skeletal muscle is affected by sarcopenia, a progressive decline in muscle mass, strength and endurance that leads to loss of function and disability. Cell nucleus dysfunction is a possible factor contributing to sarcopenia because aging-associated alterations in mRNA and rRNA transcription/maturation machinery have been shown in several cell types including muscle cells. In this study, the distribution and density of key molecular factors involved in RNA pathways namely, nuclear actin (a motor protein and regulator of RNA transcription), 5-methyl cytosine (an epigenetic regulator of gene transcription), and ribonuclease A (an RNA degrading enzyme) were compared in different nuclear compartments of late adult and old mice myonuclei by means of ultrastructural immunocytochemistry. In all nuclear compartments, an age-related decrease of nuclear actin suggested altered chromatin structuring and impaired nucleus-to-cytoplasm transport of both mRNA and ribosomal subunits, while a decrease of 5-methyl cytosine and ribonuclease A in the nucleoli of old mice indicated an age-dependent loss of rRNA genes. These findings provide novel experimental evidence that, in the aging skeletal muscle, nuclear RNA pathways undergo impairment, likely hindering protein synthesis and contributing to the onset and progression of sarcopenia.

摘要

随着年龄的增长,骨骼肌受到肌少症的影响,这是一种肌肉质量、力量和耐力逐渐下降的疾病,导致功能丧失和残疾。细胞核功能障碍是导致肌少症的一个可能因素,因为在包括肌肉细胞在内的几种细胞类型中,已经观察到与衰老相关的 mRNA 和 rRNA 转录/成熟机制的改变。在这项研究中,通过超微结构免疫细胞化学比较了核纤层蛋白(RNA 转录的调节因子)、5-甲基胞嘧啶(基因转录的表观遗传调节剂)和核糖核酸酶 A(RNA 降解酶)等参与 RNA 途径的关键分子因子在成年后期和老年小鼠肌细胞核不同核区室中的分布和密度。在所有核区室中,核纤层蛋白的年龄相关性减少表明染色质结构发生改变,并且 mRNA 和核糖体亚基的核质转运受损,而老年小鼠核仁中 5-甲基胞嘧啶和核糖核酸酶 A 的减少表明 rRNA 基因的年龄依赖性丢失。这些发现提供了新的实验证据,表明在衰老的骨骼肌中,核 RNA 途径受到损害,可能会阻碍蛋白质合成,并导致肌少症的发生和进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f2b/8033527/28bc19d23ca3/ejh-65-2-3229-g001.jpg

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