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一种通过亲和肽控制神经营养因子 3 释放的可注射 PEG 水凝胶。

An injectable PEG hydrogel controlling neurotrophin-3 release by affinity peptides.

机构信息

Department of Biomedical Engineering, University of Michigan, 48105 Ann Arbor, MI, USA.

Kresge Hearing Research Institute, Department of Otolaryngology, Head and Neck Surgery, University of Michigan Medical School, 48109 Ann Arbor, MI, USA.

出版信息

J Control Release. 2021 Feb 10;330:575-586. doi: 10.1016/j.jconrel.2020.12.045. Epub 2020 Dec 27.

Abstract

Neurotrophin-3 growth factor can improve cochlear neuron survival, and localized delivery of this protein to the round window membrane in the middle ear may be able to reverse sensorineural hearing loss. Thus, the goal of this work was to develop an injectable hydrogel delivery system that can allow localized release of neurotrophin-3 in a controlled and sustained manner. We identified a PEG hydrogel formulation that uses thiol-vinyl sulfone Michael addition for crosslinking. This injectable formulation provides elastic hydrogels with higher mechanical rigidity, better bio-adhesion and longer residence time than Poloxamer hydrogels currently being investigated clinically for hearing loss. In vivo, PEG hydrogels induce local immune responses comparable to biocompatible Poloxamer hydrogels, yet they released payloads at a ~5-fold slower rate in the subcutaneous area. Based on this injectable hydrogel formulation, we designed an affinity-based protein release system by modifying PEG hydrogels with affinity peptides specific to neurotrophin-3 proteins. We verified the sustained release of neurotrophin-3 from peptide-conjugated PEG hydrogels resulting from the reversible interaction between peptides and proteins. The rate of affinity-controlled release depends on the polymer concentrations, the affinity of peptides and the peptide-to-protein ratios. Collectively, we developed an injectable hydrogel formulation for localized delivery of neurotrophin-3, which provides affinity-controlled release and longer delivery time compared to Poloxamer hydrogels.

摘要

神经营养因子 3 生长因子可以改善耳蜗神经元的存活,将这种蛋白质局部递送到中耳的圆窗膜上可能能够逆转感觉神经性听力损失。因此,本工作的目的是开发一种可注射水凝胶递送系统,能够以受控和持续的方式局部释放神经营养因子 3。我们确定了一种使用巯基-乙烯砜迈克尔加成进行交联的 PEG 水凝胶配方。与目前正在临床研究用于听力损失的泊洛沙姆水凝胶相比,这种可注射配方提供了具有更高机械刚性、更好生物粘附性和更长滞留时间的弹性水凝胶。在体内,PEG 水凝胶引起的局部免疫反应与生物相容性的泊洛沙姆水凝胶相当,但在皮下区域的释放速度比泊洛沙姆水凝胶慢约 5 倍。基于这种可注射水凝胶配方,我们通过用特定于神经营养因子 3 蛋白的亲和肽修饰 PEG 水凝胶,设计了一种基于亲和性的蛋白释放系统。我们验证了亲和肽修饰的 PEG 水凝胶能够持续释放神经营养因子 3,这是由于肽和蛋白之间的可逆相互作用。亲和控制释放的速度取决于聚合物浓度、肽的亲和力和肽与蛋白的比例。总的来说,我们开发了一种用于神经营养因子 3 局部递送的可注射水凝胶配方,与泊洛沙姆水凝胶相比,它提供了亲和控制释放和更长的递送时间。

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