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人类骨骼肌中Plin2表达增加与肌肉减少症和肌肉无力相关。

Increased Plin2 expression in human skeletal muscle is associated with sarcopenia and muscle weakness.

作者信息

Conte Maria, Vasuri Francesco, Trisolino Giovanni, Bellavista Elena, Santoro Aurelia, Degiovanni Alessio, Martucci Ermanno, D'Errico-Grigioni Antonia, Caporossi Daniela, Capri Miriam, Maier Andrea B, Seynnes Olivier, Barberi Laura, Musarò Antonio, Narici Marco V, Franceschi Claudio, Salvioli Stefano

机构信息

Department of Experimental, Diagnostic and Specialty Medicine and Interdepartmental Centre L Galvani, CIG, University of Bologna, Bologna, Italy.

出版信息

PLoS One. 2013 Aug 15;8(8):e73709. doi: 10.1371/journal.pone.0073709. eCollection 2013.

Abstract

Human aging is associated with a progressive loss of muscle mass and strength and a concomitant fat accumulation in form of inter-muscular adipose tissue, causing skeletal muscle function decline and immobilization. Fat accumulation can also occur as intra-muscular triglycerides (IMTG) deposition in lipid droplets, which are associated with perilipin proteins, such as Perilipin2 (Plin2). It is not known whether Plin2 expression changes with age and if this has consequences on muscle mass and strength. We studied the expression of Plin2 in the vastus lateralis (VL) muscle of both healthy subjects and patients affected by lower limb mobility limitation of different age. We found that Plin2 expression increases with age, this phenomenon being particularly evident in patients. Moreover, Plin2 expression is inversely correlated with quadriceps strength and VL thickness. To investigate the molecular mechanisms underpinning this phenomenon, we focused on IGF-1/p53 network/signalling pathway, involved in muscle physiology. We found that Plin2 expression strongly correlates with increased p53 activation and reduced IGF-1 expression. To confirm these observations made on humans, we studied mice overexpressing muscle-specific IGF-1, which are protected from sarcopenia. These mice resulted almost negative for the expression of Plin2 and p53 at two years of age. We conclude that fat deposition within skeletal muscle in form of Plin2-coated lipid droplets increases with age and is associated with decreased muscle strength and thickness, likely through an IGF-1- and p53-dependent mechanism. The data also suggest that excessive intramuscular fat accumulation could be the initial trigger for p53 activation and consequent loss of muscle mass and strength.

摘要

人类衰老与肌肉质量和力量的逐渐丧失以及肌肉间脂肪组织形式的脂肪堆积同时发生,导致骨骼肌功能下降和活动受限。脂肪堆积也可表现为肌内甘油三酯(IMTG)在脂滴中的沉积,这些脂滴与脂联素蛋白相关,如脂联素2(Plin2)。目前尚不清楚Plin2的表达是否随年龄变化,以及这是否会对肌肉质量和力量产生影响。我们研究了健康受试者和不同年龄下肢活动受限患者的股外侧肌(VL)中Plin2的表达。我们发现Plin2的表达随年龄增加,这种现象在患者中尤为明显。此外,Plin2的表达与股四头肌力量和VL厚度呈负相关。为了研究这一现象背后的分子机制,我们聚焦于参与肌肉生理学的IGF-1/p53网络/信号通路。我们发现Plin2的表达与p53激活增加和IGF-1表达降低密切相关。为了证实对人类的这些观察结果,我们研究了过表达肌肉特异性IGF-1的小鼠,这些小鼠可免受肌肉减少症的影响。这些小鼠在两岁时Plin2和p53的表达几乎为阴性。我们得出结论,以Plin2包被的脂滴形式存在的骨骼肌内脂肪沉积随年龄增加,可能通过IGF-1和p53依赖的机制与肌肉力量和厚度降低相关。数据还表明,肌肉内脂肪过度堆积可能是p53激活以及随后肌肉质量和力量丧失的初始触发因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f16c/3744478/ec94c32defc0/pone.0073709.g001.jpg

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