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硫化物是卫星细胞分化和肌肉再生的生长因子信号调节剂。

Sulfs are regulators of growth factor signaling for satellite cell differentiation and muscle regeneration.

作者信息

Langsdorf Aliete, Do Anh-Tri, Kusche-Gullberg Marion, Emerson Charles P, Ai Xingbin

机构信息

Boston Biomedical Research Institute, Watertown, Massachusetts 02472, USA.

出版信息

Dev Biol. 2007 Nov 15;311(2):464-77. doi: 10.1016/j.ydbio.2007.08.053. Epub 2007 Sep 7.

Abstract

Heparan sulfate proteoglycans (HSPGs) are required during muscle regeneration for regulating extracellular signaling pathways. HSPGs interact with growth factors and receptors through heparan sulfate (HS) chains. However, the regulatory mechanisms that control HS sulfation to affect the growth factor-dependent proliferation and differentiation of satellite cells are yet unknown. Here we report the essential functions of extracellular HS 6-O-endosulfatases (Sulfs) during muscle regeneration. We show that quiescent and activated satellite cells differentially express mouse Sulf1 (MSulf1) and MSulf2. MSulfs are not required for the formation of skeletal muscles and satellite cells, but they have redundant, essential roles to promote muscle regeneration, as MSulf double mutant mice exhibit delayed myogenic differentiation and prolonged Pax7 expression after cardiotoxin-induced skeletal muscle injury, while single MSulf knockouts regenerate normally. HS structural analysis demonstrates that Sulfs are regulatory HS-modifying enzymes that control HS 6-O-desulfation of activated satellite cells. Mechanistically, we show that MSulfs repress FGF2 signaling in activated satellite cells, leading us to propose that MSulfs are growth factor signaling sensors to control the proliferation to differentiation switch of satellite cells to initiate differentiation during regeneration. Our results establish Sulfs as essential regulators of HS-dependent growth factor signaling in the adult muscle stem cell niche.

摘要

硫酸乙酰肝素蛋白聚糖(HSPGs)在肌肉再生过程中对于调节细胞外信号通路是必需的。HSPGs通过硫酸乙酰肝素(HS)链与生长因子和受体相互作用。然而,控制HS硫酸化以影响卫星细胞依赖生长因子的增殖和分化的调控机制尚不清楚。在此,我们报道了细胞外HS 6-O-硫酸酯酶(Sulfs)在肌肉再生过程中的重要功能。我们发现静止和活化的卫星细胞差异表达小鼠Sulf1(MSulf1)和MSulf2。MSulfs对于骨骼肌和卫星细胞的形成不是必需的,但它们在促进肌肉再生方面具有冗余的重要作用,因为MSulf双突变小鼠在心脏毒素诱导的骨骼肌损伤后表现出延迟的肌源性分化和延长的Pax7表达,而单个MSulf基因敲除小鼠能够正常再生。HS结构分析表明,Sulfs是调控HS修饰的酶,可控制活化卫星细胞的HS 6-O-去硫酸化。从机制上讲,我们发现MSulfs在活化卫星细胞中抑制FGF2信号传导,这使我们提出MSulfs是生长因子信号传感器,可控制卫星细胞的增殖到分化转换,从而在再生过程中启动分化。我们的结果确立了Sulfs作为成年肌肉干细胞微环境中HS依赖的生长因子信号的重要调节因子。

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