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白细胞介素-15 促进人体肌生成,并减轻 TNFα 对肌管发育的有害影响。

IL-15 promotes human myogenesis and mitigates the detrimental effects of TNFα on myotube development.

机构信息

Institute of Inflammation and Ageing, MRC-ARUK Centre for Musculoskeletal Ageing Research, University of Birmingham, Birmingham, UK.

FRAME Alternatives Laboratory, Faculty of Medicine & Health Sciences, University of Nottingham, Nottingham, UK.

出版信息

Sci Rep. 2017 Oct 11;7(1):12997. doi: 10.1038/s41598-017-13479-w.

Abstract

Studies in murine cell lines and in mouse models suggest that IL-15 promotes myogenesis and may protect against the inflammation-mediated skeletal muscle atrophy which occurs in sarcopenia and cachexia. The effects of IL-15 on human skeletal muscle growth and development remain largely uncharacterised. Myogenic cultures were isolated from the skeletal muscle of young and elderly subjects. Myoblasts were differentiated for 8 d, with or without the addition of recombinant cytokines (rIL-15, rTNFα) and an IL-15 receptor neutralising antibody. Although myotubes were 19% thinner in cultures derived from elderly subjects, rIL-15 increased the thickness of myotubes (MTT) from both age groups to a similar extent. Neutralisation of the high-affinity IL-15 receptor binding subunit, IL-15rα in elderly myotubes confirmed that autocrine concentrations of IL-15 also support myogenesis. Co-incubation of differentiating myoblasts with rIL-15 and rTNFα, limited the reduction in MTT and nuclear fusion index (NFI) associated with rTNFα stimulation alone. IL-15rα neutralisation and rTNFα decreased MTT and NFI further. This, coupled with our observation that myotubes secrete IL-15 in response to TNFα stimulation supports the notion that IL-15 serves to mitigate inflammatory skeletal muscle loss. IL-15 may be an effective therapeutic target for the attenuation of inflammation-mediated skeletal muscle atrophy.

摘要

在鼠类细胞系和小鼠模型中的研究表明,IL-15 可促进肌生成,并可能预防在肌肉减少症和恶病质中发生的炎症介导的骨骼肌萎缩。IL-15 对人类骨骼肌生长和发育的影响在很大程度上仍未得到充分描述。从年轻和老年受试者的骨骼肌中分离出成肌细胞培养物。肌母细胞分化 8 天,有或没有添加重组细胞因子(rIL-15、rTNFα)和 IL-15 受体中和抗体。尽管源自老年受试者的培养物中的肌管薄 19%,但 rIL-15 可使来自两个年龄组的肌管(MTT)增粗到相似的程度。在老年肌管中中和高亲和力的 IL-15 受体结合亚基 IL-15rα 证实,内源性 IL-15 浓度也支持肌生成。将分化的成肌细胞与 rIL-15 和 rTNFα 共同孵育,可限制 rTNFα 单独刺激引起的 MTT 和核融合指数(NFI)的降低。IL-15rα 中和和 rTNFα 进一步降低了 MTT 和 NFI。这一点,再加上我们观察到肌管在受到 TNFα 刺激时会分泌 IL-15,支持了 IL-15 可减轻炎症性骨骼肌丢失的观点。IL-15 可能是减轻炎症介导的骨骼肌萎缩的有效治疗靶点。

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