首页> 外文期刊>Biomaterials >Synergistic effects of tethered growth factors and adhesion ligands on DNA synthesis and function of primary hepatocytes cultured on soft synthetic hydrogels.
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Synergistic effects of tethered growth factors and adhesion ligands on DNA synthesis and function of primary hepatocytes cultured on soft synthetic hydrogels.

机译:拴系生长因子和粘附配体对在软合成水凝胶上培养的原代肝细胞DNA合成和功能的协同作用。

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摘要

The composition, presentation, and spatial orientation of extracellular matrix molecules and growth factors are key regulators of cell behavior. Here, we used self-assembling peptide nanofiber gels as a modular scaffold to investigate how fibronectin-derived adhesion ligands and different modes of epidermal growth factor (EGF) presentation synergistically regulate multiple facets of primary rat hepatocyte behavior in the context of a soft gel. In the presence of soluble EGF, inclusion of dimeric RGD and the heparin binding domain from fibronectin (HB) increased hepatocyte aggregation, spreading, and metabolic function compared to unmodified gels or gels modified with a single motif, but unlike rigid substrates, gels failed to induce DNA synthesis. Tethered EGF dramatically stimulated cell aggregation and spreading under all adhesive ligand conditions and also preserved metabolic function. Surprisingly, tethered EGF elicited DNA synthesis on gels with RGD and HB. Phenotypic differences between soluble and tethered EGF stimulation of cells on peptide gels are correlated with differences in expression and phosphorylation the EGF receptor and its heterodimerization partner ErbB2, and activation of the downstream signaling node ERK1/2. These modular matrices reveal new facets of hepatocellular biology in culture and may be more broadly useful in culture of other soft tissues.
机译:细胞外基质分子和生长因子的组成,表现和空间取向是细胞行为的关键调节因子。在这里,我们使用自组装肽纳米纤维凝胶作为模块化支架,以研究纤连蛋白衍生的粘附配体和不同模式的表皮生长因子(EGF)表现如何在软凝胶的情况下协同调节原代大鼠肝细胞行为的多个方面。与未修饰的凝胶或具有单个基序修饰的凝胶相比,在存在可溶性EGF的情况下,包含二聚体RGD和来自纤连蛋白(HB)的肝素结合域会增加肝细胞的聚集,扩散和代谢功能,但与刚性底物不同,该凝胶无法诱导DNA合成。束缚的EGF在所有粘附配体条件下均能显着刺激细胞聚集和扩散,并保留了新陈代谢功能。出乎意料的是,拴在一起的EGF在带有RGD和HB的凝胶上引发DNA合成。肽凝胶上细胞的可溶性和束缚性EGF刺激之间的表型差异与EGF受体及其异二聚体伴侣ErbB2的表达和磷酸化差异以及下游信号传导节点ERK1 / 2的激活相关。这些模块化矩阵揭示了培养中肝细胞生物学的新面貌,在其他软组织的培养中可能会更广泛地发挥作用。

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