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透明质酸合成与成肌作用:成肌分化过程中透明质酸合成的一个要求,与细胞外基质形成无关。

Hyaluronan synthesis and myogenesis: a requirement for hyaluronan synthesis during myogenic differentiation independent of pericellular matrix formation.

机构信息

Murdoch Children's Research Institute, Royal Children's Hospital, Parkville, Victoria 3052, Australia.

出版信息

J Biol Chem. 2013 May 3;288(18):13006-21. doi: 10.1074/jbc.M113.453209. Epub 2013 Mar 14.

Abstract

Exogenous hyaluronan is known to alter muscle precursor cell proliferation, migration, and differentiation, ultimately inhibiting myogenesis in vitro. The aim of the current study was to investigate the role of endogenous hyaluronan synthesis during myogenesis. In quantitative PCR studies, the genes responsible for synthesizing hyaluronan were found to be differentially regulated during muscle growth, repair, and pathology. Although all Has genes (Has1, Has2, and Has3) were differentially regulated in these models, only Has2 gene expression consistently associated with myogenic differentiation. During myogenic differentiation in vitro, Has2 was the most highly expressed of the synthases and increased after induction of differentiation. To test whether this association between Has2 expression and myogenesis relates to a role for Has2 in myoblast differentiation and fusion, C2C12 myoblasts were depleted of Has2 by siRNA and induced to differentiate. Depletion of Has2 inhibited differentiation and caused a loss of cell-associated hyaluronan and the hyaluronan-dependent pericellular matrix. The inhibition of differentiation caused by loss of hyaluronan was confirmed with the hyaluronan synthesis inhibitor 4-methylumbelliferone. In hyaluronan synthesis-blocked cultures, restoration of the pericellular matrix could be achieved through the addition of exogenous hyaluronan and the proteoglycan versican, but this was not sufficient to restore differentiation to control levels. These data indicate that intrinsic hyaluronan synthesis is necessary for myoblasts to differentiate and form syncytial muscle cells, but the hyaluronan-dependent pericellular matrix is not sufficient to support differentiation alone; additional hyaluronan-dependent cell functions that are yet unknown may be required for myogenic differentiation.

摘要

外源性透明质酸已知会改变肌肉前体细胞的增殖、迁移和分化,最终抑制体外的肌生成。本研究的目的是研究内源性透明质酸合成在肌生成过程中的作用。在定量 PCR 研究中,发现负责合成透明质酸的基因在肌肉生长、修复和病理过程中存在差异调控。尽管所有 Has 基因(Has1、Has2 和 Has3)在这些模型中均存在差异调控,但只有 Has2 基因表达与肌生成分化一致相关。在体外肌生成分化过程中,Has2 是合成酶中表达最高的,并且在诱导分化后增加。为了测试 Has2 表达与肌生成之间的这种关联是否与 Has2 在成肌细胞分化和融合中的作用有关,通过 siRNA 耗尽 C2C12 成肌细胞中的 Has2 并诱导其分化。Has2 的耗竭抑制了分化,并导致细胞相关透明质酸和透明质酸依赖性细胞外基质的丧失。通过透明质酸合成抑制剂 4-甲基伞形酮证实了透明质酸丧失引起的分化抑制。在透明质酸合成阻断的培养物中,通过添加外源性透明质酸和蛋白聚糖 versican 可以恢复细胞外基质,但这不足以将分化恢复到对照水平。这些数据表明,内源性透明质酸合成对于成肌细胞分化和形成合胞体肌肉细胞是必需的,但透明质酸依赖性细胞外基质本身不足以支持分化;可能需要尚未知的其他依赖透明质酸的细胞功能来进行肌生成分化。

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