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Zwitterionic PEG-PC Hydrogels Modulate the Foreign Body Response in a Modulus-Dependent Manner

机译:双层PEG-PC水凝胶以模数依赖性方式调节异物响应

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Reducing the foreign body response (FBR) to implanted biomaterials will enhance their performance in tissue engineering. Poly(ethylene glycol) (PEG) hydrogels are increasingly popular for this application due to their low cost, ease of use, and the ability to tune their compliance via molecular weight and cross-linking densities. PEG hydrogels can elicit chronic inflammation in vivo, but recent evidence has suggested that extremely hydrophilic, zwitterionic materials and particles can evade the immune system. To combine the advantages of PEG-based hydrogels with the hydrophilicity of zwitterions, we synthesized hydrogels with comonomers PEG and the zwitterion phosphorylcholine (PC). Recent evidence suggests that stiff hydrogels elicit increased immune cell adhesion to hydrogels, which we attempted to reduce by increasing hydrogel hydrophilicity. Surprisingly, hydrogels with the highest amount of zwitterionic comonomer elicited the highest FBR. Lowering the hydrogel modulus (165 to 3 kPa), or PC content (20 to 0 wt %), mitigated this effect. A high density of macrophages was found at the surface of implants associated with a high FBR, and mass spectrometry analysis of the proteins adsorbed to these gels implicated extracellular matrix, immune response, and cell adhesion protein categories as drivers of macrophage recruitment. Overall, we show that modulus regulates macrophage adhesion to zwitterionic-PEG hydrogels, and demonstrate that chemical modifications to hydrogels should be studied in parallel with their physical properties to optimize implant design.
机译:减少对植入生物材料的异物反应(FBR)将增强它们在组织工程中的性能。由于它们的低成本,易用性以及通过分子量和交联密度调谐其遵守能力,聚(乙二醇)(PEG)水凝胶越来越受欢迎。 PEG水凝胶可以在体内引发慢性炎症,但最近的证据表明,极其亲水,两性离子材料和颗粒可以避免免疫系统。结合PEG的水凝胶与两性而亲水性的优点,我们用共聚单体PEG和两性离子磷胆碱(PC)合成水凝胶。最近的证据表明,僵硬的水凝胶引发了对水凝胶的增加的免疫细胞粘附,我们试图通过增加水凝胶亲水性降低。令人惊讶的是,具有最多的两性离子共聚单体的水凝胶引发了最高的FBR。降低水凝胶模量(165至3kPa),或Pc含量(20至0wt%),减轻了这种效果。在与高FBR相关的植入物表面上发现了高密度的巨噬细胞,以及吸附于这些凝胶的蛋白质的质谱分析涉及巨噬细胞招募的司机的细胞外基质,免疫应答和细胞粘附蛋白类别。总体而言,模量调节巨噬细胞粘附到枯过硫-PEG水凝胶,并证明应与其物理性质并行研究对水凝胶的化学修饰以优化植入物设计。

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