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采用蛋白质组学和遗传学方法评估发育性肌肉萎缩。

Integration of proteomic and genetic approaches to assess developmental muscle atrophy.

机构信息

Department of Biochemistry and Molecular Biophysics, Kansas State University, Manhattan, KS 66506, USA.

出版信息

J Exp Biol. 2021 Nov 1;224(21). doi: 10.1242/jeb.242698. Epub 2021 Nov 5.

Abstract

Muscle atrophy, or a decline in muscle protein mass, is a significant problem in the aging population and in numerous disease states. Unraveling molecular signals that trigger and promote atrophy may lead to a better understanding of treatment options; however, there is no single cause of atrophy identified to date. To gain insight into this problem, we chose to investigate changes in protein profiles during muscle atrophy in Manduca sexta and Drosophila melanogaster. The use of insect models provides an interesting parallel to probe atrophic mechanisms as these organisms undergo a normal developmental atrophy process during the pupal transition stage. Leveraging the inherent advantages of each model organism, we first defined protein signature changes during M. sexta intersegmental muscle (ISM) atrophy and then used genetic approaches to confirm their functional importance in the D. melanogaster dorsal internal oblique muscles (DIOMs). Our data reveal an upregulation of proteasome and peptidase components and a general downregulation of proteins that regulate actin filament formation. Surprisingly, thick filament proteins that comprise the A-band are increased in abundance, providing support for the ordered destruction of myofibrillar components during developmental atrophy. We also uncovered the actin filament regulator ciboulot (Cib) as a novel regulator of muscle atrophy. These insights provide a framework towards a better understanding of global changes that occur during atrophy and may eventually lead to therapeutic targets.

摘要

肌肉萎缩,即肌肉蛋白质量下降,是老年人群体和多种疾病状态中的一个重大问题。解析引发并促进萎缩的分子信号可能有助于更好地了解治疗选择;然而,迄今为止尚未确定导致萎缩的单一原因。为了深入了解这一问题,我们选择研究曼陀罗蚕和黑腹果蝇的肌肉萎缩过程中的蛋白质谱变化。使用昆虫模型提供了一个有趣的平行途径来探究萎缩机制,因为这些生物体在蛹转变阶段经历正常的发育性萎缩过程。利用每个模式生物的固有优势,我们首先定义了曼陀罗蚕体节间肌肉(ISM)萎缩过程中的蛋白质特征变化,然后使用遗传方法确认它们在黑腹果蝇背内斜肌(DIOM)中的功能重要性。我们的数据揭示了蛋白酶体和肽酶成分的上调,以及调节肌动蛋白丝形成的蛋白质的普遍下调。令人惊讶的是,构成 A 带的粗肌丝蛋白的丰度增加,为肌原纤维成分在发育性萎缩过程中的有序破坏提供了支持。我们还发现了肌动蛋白丝调节剂 ciboulot(Cib)是肌肉萎缩的一个新的调节因子。这些发现为理解萎缩过程中发生的全局变化提供了一个框架,并可能最终导致治疗靶点的出现。

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