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慢性低频刺激快肌的蛋白质组学分析

Proteomic profiling of chronic low-frequency stimulated fast muscle.

作者信息

Donoghue Pamela, Doran Phil, Wynne Kieran, Pedersen Kasper, Dunn Michael J, Ohlendieck Kay

机构信息

Proteome Research Centre, UCD Conway Institute, University College Dublin, Dublin, Ireland.

出版信息

Proteomics. 2007 Sep;7(18):3417-30. doi: 10.1002/pmic.200700262.

Abstract

Skeletal muscle fibre transitions occur in many biological processes, in response to alterations in neuromuscular activity, in muscular disorders, during age-induced muscle wasting and in myogenesis. It was therefore of interest to perform a comprehensive proteomic profiling of muscle transformation. Chronic low-frequency stimulation of the rabbit tibialis anterior muscle represents an established model system for studying the response of fast fibres to enhanced neuromuscular activity under conditions of maximum activation. We have conducted a DIGE analysis of unstimulated control specimens versus 14- and 60-day conditioned muscles. A differential expression pattern was observed for 41 protein species with 29 increased and 12 decreased muscle proteins. Identified classes of proteins that are changed during the fast-to-slow transition process belong to the contractile machinery, ion homeostasis, excitation-contraction coupling, capillarization, metabolism and stress response. Results from immunoblotting agreed with the conversion of the metabolic, regulatory and contractile molecular apparatus to support muscle fibres with slower twitch characteristics. Besides confirming established muscle elements as reliable transition markers, this proteomics-based study has established the actin-binding protein cofilin-2 and the endothelial marker transgelin as novel biomarkers for evaluating muscle transformation.

摘要

骨骼肌纤维转变发生在许多生物学过程中,响应神经肌肉活动的改变、肌肉疾病、年龄诱导的肌肉萎缩以及肌生成过程。因此,对肌肉转变进行全面的蛋白质组学分析很有意义。对兔胫前肌进行慢性低频刺激是一种成熟的模型系统,用于研究在最大激活条件下快肌纤维对增强的神经肌肉活动的反应。我们对未刺激的对照标本与14天和60天条件化肌肉进行了差异凝胶电泳(DIGE)分析。观察到41种蛋白质的差异表达模式,其中29种肌肉蛋白质增加,12种减少。在快肌向慢肌转变过程中发生变化的已鉴定蛋白质类别属于收缩机制、离子稳态、兴奋-收缩偶联、毛细血管化、代谢和应激反应。免疫印迹结果与代谢、调节和收缩分子装置的转变一致,以支持具有较慢收缩特性的肌肉纤维。除了确认已有的肌肉成分作为可靠的转变标志物外,这项基于蛋白质组学的研究还确立了肌动蛋白结合蛋白丝切蛋白-2和内皮标志物转胶蛋白作为评估肌肉转变的新型生物标志物。

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