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免疫系统的再生功能:对肌肉干细胞的调节

Regenerative function of immune system: Modulation of muscle stem cells.

作者信息

Saini Jasdeep, McPhee Jamie S, Al-Dabbagh Sarah, Stewart Claire E, Al-Shanti Nasser

机构信息

Healthcare Science Research Institute, School of Healthcare Science Manchester Metropolitan University, John Dalton Building, Chester Street, M1 5GD Manchester, UK.

Research Institute for Sport & Exercise Sciences, School of Sport and Exercise Sciences, Tom Reilly Building, Byrom Street Campus, Liverpool John Moores University, Liverpool L3 3AF, UK.

出版信息

Ageing Res Rev. 2016 May;27:67-76. doi: 10.1016/j.arr.2016.03.006. Epub 2016 Mar 31.

Abstract

Ageing is characterised by progressive deterioration of physiological systems and the loss of skeletal muscle mass is one of the most recognisable, leading to muscle weakness and mobility impairments. This review highlights interactions between the immune system and skeletal muscle stem cells (widely termed satellite cells or myoblasts) to influence satellite cell behaviour during muscle regeneration after injury, and outlines deficits associated with ageing. Resident neutrophils and macrophages in skeletal muscle become activated when muscle fibres are damaged via stimuli (e.g. contusions, strains, avulsions, hyperextensions, ruptures) and release high concentrations of cytokines, chemokines and growth factors into the microenvironment. These localised responses serve to attract additional immune cells which can reach in excess of 1×10(5) immune cell/mm(3) of skeletal muscle in order to orchestrate the repair process. T-cells have a delayed response, reaching peak activation roughly 4 days after the initial damage. The cytokines and growth factors released by activated T-cells play a key role in muscle satellite cell proliferation and migration, although the precise mechanisms of these interactions remain unclear. T-cells in older people display limited ability to activate satellite cell proliferation and migration which is likely to contribute to insufficient muscle repair and, consequently, muscle wasting and weakness. If the factors released by T-cells to activate satellite cells can be identified, it may be possible to develop therapeutic agents to enhance muscle regeneration and reduce the impact of muscle wasting during ageing and disease.

摘要

衰老的特征是生理系统的逐渐衰退,骨骼肌质量的丧失是最明显的特征之一,会导致肌肉无力和行动障碍。本综述强调了免疫系统与骨骼肌干细胞(通常称为卫星细胞或成肌细胞)之间的相互作用,以影响损伤后肌肉再生过程中卫星细胞的行为,并概述了与衰老相关的缺陷。当肌纤维通过刺激(如挫伤、拉伤、撕脱伤、过度伸展、破裂)受损时,骨骼肌中的驻留中性粒细胞和巨噬细胞被激活,并向微环境中释放高浓度的细胞因子、趋化因子和生长因子。这些局部反应有助于吸引更多的免疫细胞,这些免疫细胞在每立方毫米骨骼肌中可达超过1×10(5)个,以协调修复过程。T细胞反应延迟,在初始损伤后约4天达到激活峰值。活化的T细胞释放的细胞因子和生长因子在肌肉卫星细胞增殖和迁移中起关键作用,但这些相互作用的确切机制仍不清楚。老年人中的T细胞激活卫星细胞增殖和迁移的能力有限,这可能导致肌肉修复不足,进而导致肌肉萎缩和无力。如果能够识别出T细胞释放以激活卫星细胞的因子,那么有可能开发出治疗药物来增强肌肉再生,并减少衰老和疾病期间肌肉萎缩的影响。

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