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Heparin-based coacervate of bFGF facilitates peripheral nerve regeneration by inhibiting endoplasmic reticulum stress following sciatic nerve injury

机译:基于肝素的bFGF凝聚层通过抑制坐骨神经损伤后的内质网应激促进周围神经再生

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摘要

Creating a microenvironment at the injury site that favors axonal regrowth and remyelinationis pivotal to the success of therapeutic reinnervation. The mature myelin sheath of the peripheral nervous system depends on active participation of Schwann cells to form new cytoskeletal components and tremendous amounts of relevant neurotrophic factors. In this study, we utilized a new biomaterial for growth factor delivery consisting of a biocompatible polycation, poly(ethylene argininylaspartatediglyceride) and heparin. It is capable of binding a variety of growth factors to deliver basic fibroblast growth factor (bFGF) through polyvalent ionic interactions for nerve repair. In vitro assays demonstrated that the bFGF loading efficiency reached 10 μg and this delivery vehicle could control the release of bFGF. In vivo, the coacervate enhanced bFGF bioavailability, which improved both motor and sensory function. It could also acceleratemyelinated fiber regeneration and remyelination and promote Schwann cells proliferation. Furthermore, the neuroprotective effect of bFGF-coacervate in sciatic nerve injury was associated with the alleviation of endoplasmic reticulum stress signal. This heparin-based delivery platform leads to increased bFGF loading efficiency and better controls its release, which will provide an effective strategy for peripheral nerve injury regeneration therapy.
机译:在损伤部位创造有利于轴突再生和髓鞘再生的微环境,对于治疗性神经再生的成功至关重要。周围神经系统成熟的髓鞘,取决于雪旺细胞的主动参与,以形成新的细胞骨架成分和大量相关的神经营养因子。在这项研究中,我们利用一种新的生物材料来输送生长因子,该材料包括生物相容性聚阳离子,聚(乙烯-精氨酸-丙二酸二甘油酯)和肝素。它能够结合多种生长因子,以通过神经修复的多价离子相互作用传递碱性成纤维细胞生长因子(bFGF)。体外试验表明,bFGF的加载效率达到10μg,并且该递送载体可以控制bFGF的释放。在体内,凝聚层增强了bFGF的生物利用度,从而改善了运动和感觉功能。它还可以加速髓鞘纤维再生和髓鞘再生,并促进雪旺细胞增殖。此外,bFGF凝聚层对坐骨神经损伤的神经保护作用与减轻内质网应激信号有关。这种基于肝素的递送平台可提高bFGF的加载效率并更好地控制其释放,这将为周围神经损伤的再生治疗提供有效的策略。

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