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采用生物化学方法分离肌细胞核,以确定衰老过程中肌细胞核蛋白质组的变化。

Biochemical isolation of myonuclei employed to define changes to the myonuclear proteome that occur with aging.

作者信息

Cutler Alicia A, Dammer Eric B, Doung Duc M, Seyfried Nicholas T, Corbett Anita H, Pavlath Grace K

机构信息

Department of Pharmacology, Emory University, Atlanta, GA, 30322, USA.

Graduate Program in Biochemistry, Cell and Developmental Biology, Emory University, Atlanta, GA, 30322, USA.

出版信息

Aging Cell. 2017 Aug;16(4):738-749. doi: 10.1111/acel.12604. Epub 2017 May 23.

Abstract

Skeletal muscle aging is accompanied by loss of muscle mass and strength. Examining changes in myonuclear proteins with age would provide insight into molecular processes which regulate these profound changes in muscle physiology. However, muscle tissue is highly adapted for contraction and thus comprised largely of contractile proteins making the nuclear proteins difficult to identify from whole muscle samples. By developing a method to purify myonuclei from whole skeletal muscle, we were able to collect myonuclei for analysis by flow cytometry, biochemistry, and mass spectrometry. Nuclear purification dramatically increased the number and intensity of nuclear proteins detected by mass spectrometry compared to whole tissue. We exploited this increased proteomic depth to investigate age-related changes to the myonuclear proteome. Nuclear levels of 54 of 779 identified proteins (7%) changed significantly with age; these proteins were primarily involved in chromatin maintenance and RNA processing. To determine whether the changes we detected were specific to myonuclei or were common to nuclei of excitatory tissues, we compared aging in myonuclei to aging in brain nuclei. Although several of the same processes were affected by aging in both brain and muscle nuclei, the specific proteins involved in these alterations differed between the two tissues. Isolating myonuclei allowed a deeper view into the myonuclear proteome than previously possible facilitating identification of novel age-related changes in skeletal muscle. Our technique will enable future studies into a heretofore underrepresented compartment of skeletal muscle.

摘要

骨骼肌衰老伴随着肌肉质量和力量的丧失。研究肌核蛋白随年龄的变化,将有助于深入了解调节肌肉生理学这些深刻变化的分子过程。然而,肌肉组织高度适应收缩,因此主要由收缩蛋白组成,这使得从全肌肉样本中鉴定核蛋白变得困难。通过开发一种从全骨骼肌中纯化肌核的方法,我们能够收集肌核,用于流式细胞术、生物化学和质谱分析。与全组织相比,核纯化显著增加了质谱检测到的核蛋白的数量和强度。我们利用这种增加的蛋白质组深度来研究肌核蛋白质组与年龄相关的变化。在779种已鉴定的蛋白质中,有54种(7%)的核水平随年龄显著变化;这些蛋白质主要参与染色质维持和RNA加工。为了确定我们检测到的变化是肌核特有的,还是兴奋性组织的核共有的,我们将肌核衰老与脑核衰老进行了比较。虽然大脑和肌肉核中的衰老都影响了几个相同的过程,但这两种组织中参与这些改变的特定蛋白质有所不同。分离肌核使我们能够比以往更深入地了解肌核蛋白质组,有助于识别骨骼肌中与年龄相关的新变化。我们的技术将使未来能够对骨骼肌中一个迄今代表性不足的部分进行研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ea2/5506426/997a4cdc69ce/ACEL-16-738-g001.jpg

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