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Sulfated hyaluronan alters fibronectin matrix assembly and promotes osteogenic differentiation of human bone marrow stromal cells

机译:硫酸化透明质酸改变纤连蛋白基质组装并促进人骨髓基质细胞的成骨分化

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摘要

Extracellular matrix (ECM) composition and structural integrity is one of many factors that influence cellular differentiation. Fibronectin (FN) which is in many tissues the most abundant ECM protein forms a unique fibrillary network. FN homes several binding sites for sulfated glycosaminoglycans (sGAG), such as heparin (Hep), which was previously shown to influence FN conformation and protein binding. Synthetically sulfated hyaluronan derivatives (sHA) can serve as model molecules with a well characterized sulfation pattern to study sGAG-FN interaction. Here is shown that the low-sulfated sHA (sHA1) interacts with FN and influences fibril assembly. The interaction of FN fibrils with sHA1 and Hep, but not with non-sulfated HA was visualized by immunofluorescent co-staining. FRET analysis of FN confirmed the presence of more extended fibrils in human bone marrow stromal cells (hBMSC)-derived ECM in response to sHA1 and Hep. Although both sHA1 and Hep affected FN conformation, exclusively sHA1 increased FN protein level and led to thinner fibrils. Further, only sHA1 had a pro-osteogenic effect and enhanced the activity of tissue non-specific alkaline phosphatase. We hypothesize that the sHA1-triggered change in FN assembly influences the entire ECM network and could be the underlying mechanism for the pro-osteogenic effect of sHA1 on hBMSC.
机译:细胞外基质(ECM)的组成和结构完整性是影响细胞分化的众多因素之一。纤连蛋白(FN)是许多组织中最丰富的ECM蛋白,形成独特的纤维网络。 FN驻留了硫酸化糖胺聚糖(sGAG)的几个结合位点,例如肝素(Hep),先前已证明会影响FN构象和蛋白质结合。合成硫酸化的透明质酸衍生物(sHA)可以用作模型分子,具有特征明确的硫酸化模式,以研究sGAG-FN相互作用。此处显示低硫酸盐sHA(sHA1)与FN相互作用并影响原纤维组装。通过免疫荧光共染色可观察到FN原纤维与sHA1和Hep的相互作用,但与未硫酸化的HA的相互作用不可见。 FFN的FN分析证实,人骨髓基质细胞(hBMSC)衍生的ECM对sHA1和Hep有更多延伸的原纤维存在。尽管sHA1和Hep都影响FN构象,但仅sHA1会增加FN蛋白水平并导致纤丝变薄。此外,仅sHA1具有促成骨作用,并增强了组织非特异性碱性磷酸酶的活性。我们假设sHA1触发的FN装配变化影响整个ECM网络,并且可能是sHA1对hBMSC促成骨作用的潜在机制。

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