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通过核心蛋白聚糖表达抑制成肌细胞迁移对于正常骨骼肌分化至关重要。

Inhibition of myoblast migration via decorin expression is critical for normal skeletal muscle differentiation.

作者信息

Olguin Hugo C, Santander Cristian, Brandan Enrique

机构信息

Centro de Regulación Celular y Patología, Departamento de Biologia Celular y Molecular, Facultad de Ciencias Biológicas, MIFAB, P. Universidad Católica de Chile, Santiago, Chile.

出版信息

Dev Biol. 2003 Jul 15;259(2):209-24. doi: 10.1016/s0012-1606(03)00180-5.

DOI:10.1016/s0012-1606(03)00180-5
PMID:12871697
Abstract

During limb skeletal muscle formation, committed muscle cells proliferate and differentiate in the presence of extracellular signals that stimulate or repress each process. Proteoglycans are extracellular matrix organizers and modulators of growth factor activities, regulating muscle differentiation in vitro. Previously, we characterized proteoglycan expression during early limb muscle formation and showed a spatiotemporal relation between the onset of myogenesis and the expression of decorin, an important muscle extracellular matrix component and potent regulator of TGF-beta activity. To evaluate decorin's role during in vivo differentiation in committed muscle cells, we grafted wild type and decorin-null myoblasts onto chick limb buds. The absence of decorin enhanced the migration and distribution of myoblasts in the limb, correlating with the inhibition of skeletal muscle differentiation. Both phenotypes were reverted by de novo decorin expression. In vitro, we determined that both decorin core protein and its glycosaminoglycan chain were required to reverse the migration phenotype. Results presented here suggest that the enhanced migration observed in decorin-null myoblasts may not be dependent on chemotactic growth factor signaling nor the differentiation status of the cells. Decorin may be involved in the establishment and/or coordination of a critical myoblast density, through inhibition of migration, that permits normal muscle differentiation during embryonic myogenesis.

摘要

在肢体骨骼肌形成过程中,已定向分化的肌细胞在刺激或抑制每个过程的细胞外信号存在下增殖和分化。蛋白聚糖是细胞外基质的组织者和生长因子活性的调节剂,在体外调节肌肉分化。此前,我们对早期肢体肌肉形成过程中的蛋白聚糖表达进行了表征,并显示了肌发生起始与核心蛋白聚糖(一种重要的肌肉细胞外基质成分和TGF-β活性的有效调节剂)表达之间的时空关系。为了评估核心蛋白聚糖在已定向分化的肌细胞体内分化过程中的作用,我们将野生型和缺乏核心蛋白聚糖的成肌细胞移植到鸡胚肢芽上。缺乏核心蛋白聚糖会增强成肌细胞在肢体中的迁移和分布,这与骨骼肌分化的抑制相关。这两种表型都可通过重新表达核心蛋白聚糖而恢复。在体外,我们确定核心蛋白聚糖核心蛋白及其糖胺聚糖链都需要逆转迁移表型。此处给出的结果表明,在缺乏核心蛋白聚糖的成肌细胞中观察到的迁移增强可能既不依赖于趋化性生长因子信号传导,也不依赖于细胞的分化状态。核心蛋白聚糖可能通过抑制迁移参与关键成肌细胞密度的建立和/或协调,从而在胚胎肌发生过程中允许正常的肌肉分化。

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Inhibition of myoblast migration via decorin expression is critical for normal skeletal muscle differentiation.通过核心蛋白聚糖表达抑制成肌细胞迁移对于正常骨骼肌分化至关重要。
Dev Biol. 2003 Jul 15;259(2):209-24. doi: 10.1016/s0012-1606(03)00180-5.
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The extracellular matrix regulates the effect of decorin and transforming growth factor beta-2 (TGF-β2) on myoblast migration.细胞外基质调节核心蛋白聚糖和转化生长因子β2(TGF-β2)对成肌细胞迁移的影响。
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