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生物工程化骨骼肌作为肌肉衰老和再生的模型。

Bioengineered Skeletal Muscle as a Model of Muscle Aging and Regeneration.

机构信息

Department of Chemical and Biological Engineering, University at Buffalo, The State University of New York, Buffalo, New York, USA.

Department of Biomedical Engineering, University at Buffalo, The State University of New York, Buffalo, New York, USA.

出版信息

Tissue Eng Part A. 2021 Jan;27(1-2):74-86. doi: 10.1089/ten.TEA.2020.0005. Epub 2020 Jun 16.

Abstract

With age, adult skeletal muscle (SkM) is known to decrease in muscle mass, strength, and functional capacity, a state known as sarcopenia. Here we developed an three-dimensional (3D) bioengineered senescent SkM tissue using primary human myoblasts. These tissues exhibited the characteristics of atrophied muscle, including expression of senescent genes, decreased number of satellite cells, reduced number and size of myofibers, and compromised metabolism and calcium flux. As a result, senescent SkM tissues showed impaired ability to generate force in response to electrical stimulation compared with young tissues. Furthermore, in contrast to young SkM tissues, senescent tissues failed to regenerate in response to injury, possibly as a result of persistent apoptosis and failure to initiate a proliferation program. Our findings suggest that 3D senescent SkM may provide a powerful model for studying aging and a platform for drug testing and discovery of therapeutic compounds to improve the function of sarcopenic muscle. Impact statement Skeletal muscle (SkM) plays important physiological roles and has significant regenerative capacity. However, aged SkM lose their functionality and regeneration ability. In this article, we present a senescent human bioengineering SkM tissue model that can be used to investigate senescence, metabolic or genetic diseases that inflict SkM, and to test various strategies including novel small molecules that restore muscle function and promote regeneration. One key limitation of two-dimensional cell culture system is the detachment of contractile myotubes from the surface over time, thereby limiting the evaluation of myogenic function. Here we use primary human myoblasts, which exhibit all major hallmarks of aging to mimic the organization and function of native muscle. Using this system, we were able to measure the contractile function, calcium transients, and regeneration capacity of SkM tissues. We also evaluated the response of senescent SkM tissues to injury and their ability to regenerate and recover, compared with "young" tissues. Our results suggest that three-dimensional constructs enable organization of contractile units including myosin and actin filaments, thereby providing a powerful platform for the quantitative assessment of muscle myotubes in response to injury, genetic or metabolic disorders, or pharmacological testing.

摘要

随着年龄的增长,成人骨骼肌(SkM)的肌肉质量、力量和功能能力会下降,这种状态被称为肌肉减少症。在这里,我们使用原代人类成肌细胞开发了一种三维(3D)衰老 SkM 组织。这些组织表现出萎缩肌肉的特征,包括衰老基因的表达、卫星细胞数量减少、肌纤维数量和大小减少以及代谢和钙流受损。结果,衰老的 SkM 组织在对电刺激产生力的能力方面表现出受损,与年轻组织相比。此外,与年轻的 SkM 组织相比,衰老的组织在受伤后无法再生,这可能是由于持续的细胞凋亡和未能启动增殖程序所致。我们的研究结果表明,3D 衰老的 SkM 可能为研究衰老以及药物测试和发现改善肌肉减少症肌肉功能的治疗化合物提供一个强大的模型。影响陈述骨骼肌(SkM)发挥着重要的生理作用,具有显著的再生能力。然而,衰老的 SkM 会失去其功能和再生能力。在本文中,我们提出了一种衰老的人类生物工程 SkM 组织模型,可用于研究衰老、影响 SkM 的代谢或遗传疾病,以及测试各种策略,包括恢复肌肉功能和促进再生的新型小分子。二维细胞培养系统的一个关键限制是随着时间的推移,收缩性肌管会从表面脱离,从而限制了对成肌功能的评估。在这里,我们使用原代人类成肌细胞,它们表现出衰老的所有主要特征,以模拟天然肌肉的组织和功能。使用该系统,我们能够测量 SkM 组织的收缩功能、钙瞬变和再生能力。我们还评估了衰老的 SkM 组织对损伤的反应及其与“年轻”组织相比的再生和恢复能力。我们的研究结果表明,三维构建体能够组织收缩单位,包括肌球蛋白和肌动蛋白丝,从而为定量评估肌肉肌管对损伤、遗传或代谢紊乱或药物测试的反应提供了强大的平台。

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