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Sulfated hydrogel matrices direct mitogenicity and maintenance of chondrocyte phenotype through activation of FGF signaling

机译:硫酸化水凝胶基质通过激活FGF信号传导指导有丝分裂性和软骨细胞表型的维持

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摘要

Deciphering the roles of chemical and physical features of the extracellular matrix (ECM) is vital for developing biomimetic materials with desired cellular responses in regenerative medicine. Here, we demonstrate that sulfation of biopolymers, mimicking the proteoglycans in native tissues, induces mitogenicity, chondrogenic phenotype, and suppresses catabolic activity of chondrocytes, a cell type that resides in a highly sulfated tissue. We show through tunable modification of alginate that increased sulfation of the microenvironment promotes FGF signaling-mediated proliferation of chondrocytes in a three-dimensional (3D) matrix independent of stiffness, swelling, and porosity. Furthermore, we show for the first time that a biomimetic hydrogel acts as a 3D signaling matrix to mediate a heparan sulfate/heparin-like interaction between FGF and its receptor leading to signaling cascades inducing cell proliferation, cartilage matrix production, and suppression of de-differentiation markers. Collectively, this study reveals important insights on mimicking the ECM to guide self-renewal of cells via manipulation of distinct signaling mechanisms.
机译:破解细胞外基质(ECM)的化学和物理特征的作用对于在再生医学中开发具有所需细胞反应的仿生材料至关重要。在这里,我们证明了生物聚合物的硫酸化,模仿天然组织中的蛋白聚糖,可诱导有丝分裂性,软骨形成表型,并抑制软骨细胞的分解代谢活性,而软骨细胞是一种高度硫酸化的组织。我们通过藻酸盐的可调修饰表明,微环境的硫酸盐化增加促进了FGF信号介导的软骨细胞在三维(3D)基质中的生长,而与刚性,膨胀和孔隙率无关。此外,我们首次证明了仿生水凝胶充当3D信号基质来介导FGF及其受体之间的硫酸乙酰肝素/肝素样相互作用,从而导致信号级联反应诱导细胞增殖,软骨基质生成以及抑制去氢核糖核酸。分化标记。总的来说,这项研究揭示了模仿ECM通过操纵不同信号机制来指导细胞自我更新的重要见解。

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