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首页> 外文期刊>Biomacromolecules >Hybrid Elastin-like Polypeptide-Polyethylene Glycol (ELP-PEG) Hydrogels with Improved Transparency and Independent Control of Matrix Mechanics and Cell Ligand Density
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Hybrid Elastin-like Polypeptide-Polyethylene Glycol (ELP-PEG) Hydrogels with Improved Transparency and Independent Control of Matrix Mechanics and Cell Ligand Density

机译:具有改善的透明度和基质力学和细胞配体密度的独立控制的混合类弹性蛋白的多肽-聚乙二醇(ELP-PEG)水凝胶

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摘要

Hydrogels have been developed as extracellular matrix (ECM) mimics both for therapeutic applications and basic biological studies. In particular, elastin-like polypeptide (ELP) hydrogels, which can be tuned to mimic several biochemical and physical characteristics of native ECM, have been constructed to encapsulate various types of cells to create in vitro mimics of in vivo tissues. However, ELP hydrogels become opaque at body temperature because of ELP's lower critical solution temperature behavior. This opacity obstructs light-based observation of the morphology and behavior of encapsulated cells. In order to improve the transparency of ELP hydrogels for better imaging, we have designed a hybrid ELP-polyethylene glycol (PEG) hydrogel system that rapidly cross-links with tris(hydroxymethyl) phosphine (THP) in aqueous solution via Mannich-type condensation. As expected, addition of the hydrophilic PEG component significantly improves the light transmittance. Coherent anti-Stokes Raman scattering (CARS) microscopy reveals that the hybrid ELP-PEG hydrogels have smaller hydrophobic ELP aggregates at 37 °C. Importantly, this hydrogel platform enables independent tuning of adhesion ligand density and matrix stiffness, which is desirable for studies of cell—matrix interactions. Human fibroblasts encapsulated in these hydrogels show high viability (>98%) after 7 days of culture. High-resolution confocal microscopy of encapsulated fibroblasts reveals that the cells adopt a more spread morphology in response to higher RGD ligand concentrations and softer gel mechanics.
机译:水凝胶已被开发为细胞外基质(ECM)模仿物,用于治疗应用和基础生物学研究。特别地,可以调节成模仿天然ECM的几种生化和物理特性的弹性蛋白样多肽(ELP)水凝胶已经被构造成封装各种类型的细胞以产生体内组织的体外模拟物。但是,由于ELP的临界溶液温度行为较低,因此ELP水凝胶在体温下变得不透明。这种不透明性阻碍了基于光的封装细胞形态和行为的观察。为了提高ELP水凝胶的透明度以实现更好的成像,我们设计了一种ELP-聚乙二醇(PEG)杂化水凝胶体系,该体系通过曼尼希型缩合与水溶液中的三(羟甲基)膦(THP)快速交联。如所期望的,亲水性PEG组分的添加显着改善了透光率。相干抗斯托克斯拉曼散射(CARS)显微镜显示,杂化ELP-PEG水凝胶在37°C时具有较小的疏水性ELP聚集体。重要的是,该水凝胶平台能够独立调节粘附配体的密度和基质的刚度,这对于研究细胞与基质的相互作用是理想的。培养7天后,包裹在这些水凝胶中的人成纤维细胞显示出高生存力(> 98%)。封装的成纤维细胞的高分辨率共聚焦显微镜显示,细胞响应较高的RGD配体浓度和较软的凝胶力学而采取更分散的形态。

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