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表面结合转化生长因子-β的聚氨酯影响骨骼肌局部炎症和内质网应激。

Polyurethane conjugating TGF-β on surface impacts local inflammation and endoplasmic reticulum stress in skeletal muscle.

作者信息

Shi Dandan, Xiao Jiangwei, Gu Ruicai, Wu Gang, Liao Hua

机构信息

Department of Anatomy, Guangdong Provincial Key Laboratory of Construction and Detection in Tissue Engineering, Southern Medical University, GuangZhou, 510515, China.

School of Materials Science and Engineering, South China University of Technology, Guangzhou, 510641, China.

出版信息

J Biomed Mater Res A. 2017 Apr;105(4):1156-1165. doi: 10.1002/jbm.a.35999. Epub 2017 Feb 9.

DOI:10.1002/jbm.a.35999
PMID:28076889
Abstract

The synthesized short peptide-polymers would provide key functions for tissue regeneration and repair, through enriching bioactive molecules on polymers or releasing these molecules pre-conjugated on the materials. We have developed a degradable polyurethane (PU) bearing HSNGLPL peptide, which has affinity binding ability to transforming growth factor-betas (TGF-β). For deeply understanding spatial release of TGF-β from the PU polymers and its localized bioactivity, quartz crystal microbalance (QCM) and Elisa test were used to verify TGF-β binding capacities in vitro and in vivo. The PU polymers, with or without pre-conjugating of TGF-β, were implanted into gastronomies muscle (GN) of C57BL/6 mice, for addressing TGF-β release from the polymers and its bio-regulating function in vivo. QCM result shows that PU bearing HSNGLPL peptide has affinity binding ability to TGF-β in vitro. Intramuscular implanting experiment further supports the enrichment efficiency of TGF-β on PU polymers in vivo. The detecting data involving intramuscular inflammatory infiltration triggered by the implants, myofiber regeneration, muscular fibrosis degree, and activation of endoplasmic reticulum stress (ER stress), evidence TGF-β can be released from PU polymers, and exerts regulating effects on the material-induced inflammation. Thus, our present results suggest it is feasible to improve biocompatibility of PU polymers in vivo, by pre-bearing bioactive molecules on materials before the implanting. © 2017 Wiley Periodicals, Inc. J Biomed Mater Res Part A: 105A: 1156-1165, 2017.

摘要

合成的短肽聚合物将通过在聚合物上富集生物活性分子或释放预先结合在材料上的这些分子,为组织再生和修复提供关键功能。我们开发了一种带有HSNGLPL肽的可降解聚氨酯(PU),该肽对转化生长因子-β(TGF-β)具有亲和结合能力。为了深入了解TGF-β从PU聚合物中的空间释放及其局部生物活性,使用石英晶体微天平(QCM)和酶联免疫吸附测定(ELISA)试验在体外和体内验证TGF-β的结合能力。将预先结合或未结合TGF-β的PU聚合物植入C57BL/6小鼠的胃肌(GN)中,以研究聚合物中TGF-β的释放及其在体内的生物调节功能。QCM结果表明,带有HSNGLPL肽的PU在体外对TGF-β具有亲和结合能力。肌肉内植入实验进一步支持了TGF-β在体内对PU聚合物的富集效率。涉及植入物引发的肌肉内炎症浸润、肌纤维再生、肌肉纤维化程度和内质网应激(ER应激)激活的检测数据证明,TGF-β可以从PU聚合物中释放出来,并对材料诱导的炎症发挥调节作用。因此,我们目前的结果表明,在植入前在材料上预先负载生物活性分子以提高PU聚合物在体内的生物相容性是可行的。©2017威利期刊公司。《生物医学材料研究杂志》A部分:105A:1156 - 1165,2017年。

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