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一种导电超分子水凝胶可创建理想的内源性微环境以促进脊髓损伤修复。

A conductive supramolecular hydrogel creates ideal endogenous niches to promote spinal cord injury repair.

作者信息

Yang Biao, Liang Chengzhen, Chen Di, Cheng Feng, Zhang Yuang, Wang Shaoke, Shu Jiawei, Huang Xianpeng, Wang Jingkai, Xia Kaishun, Ying Liwei, Shi Kesi, Wang Chenggui, Wang Xuhua, Li Fangcai, Zhao Qian, Chen Qixin

机构信息

Department of Orthopedics Surgery, The Second Affiliated Hospital, School of Medicine, Zhejiang University, Hangzhou, 310009, Zhejiang, China.

Orthopedics Research Institute of Zhejiang University, Hangzhou, 310009, Zhejiang, China.

出版信息

Bioact Mater. 2021 Dec 23;15:103-119. doi: 10.1016/j.bioactmat.2021.11.032. eCollection 2022 Sep.

Abstract

The current effective method for treatment of spinal cord injury (SCI) is to reconstruct the biological microenvironment by filling the injured cavity area and increasing neuronal differentiation of neural stem cells (NSCs) to repair SCI. However, the method is characterized by several challenges including irregular wounds, and mechanical and electrical mismatch of the material-tissue interface. In the current study, a unique and facile agarose/gelatin/polypyrrole (Aga/Gel/PPy, AGP3) hydrogel with similar conductivity and modulus as the spinal cord was developed by altering the concentration of Aga and PPy. The gelation occurred through non-covalent interactions, and the physically crosslinked features made the AGP3 hydrogels injectable. In vitro cultures showed that AGP3 hydrogel exhibited excellent biocompatibility, and promoted differentiation of NSCs toward neurons whereas it inhibited over-proliferation of astrocytes. The in vivo implanted AGP3 hydrogel completely covered the tissue defects and reduced injured cavity areas. In vivo studies further showed that the AGP3 hydrogel provided a biocompatible microenvironment for promoting endogenous neurogenesis rather than glial fibrosis formation, resulting in significant functional recovery. RNA sequencing analysis further indicated that AGP3 hydrogel significantly modulated expression of neurogenesis-related genes through intracellular Ca signaling cascades. Overall, this supramolecular strategy produces AGP3 hydrogel that can be used as favorable biomaterials for SCI repair by filling the cavity and imitating the physiological properties of the spinal cord.

摘要

目前治疗脊髓损伤(SCI)的有效方法是通过填充损伤腔隙区域和增加神经干细胞(NSCs)的神经元分化来重建生物微环境,以修复脊髓损伤。然而,该方法存在几个挑战,包括伤口不规则以及材料-组织界面的机械和电学不匹配。在本研究中,通过改变琼脂糖(Aga)和聚吡咯(PPy)的浓度,开发了一种具有与脊髓相似电导率和模量的独特且简便的琼脂糖/明胶/聚吡咯(Aga/Gel/PPy,AGP3)水凝胶。凝胶化通过非共价相互作用发生,物理交联特性使AGP3水凝胶具有可注射性。体外培养表明,AGP3水凝胶表现出优异的生物相容性,促进神经干细胞向神经元分化,同时抑制星形胶质细胞过度增殖。体内植入的AGP3水凝胶完全覆盖组织缺损并减小损伤腔隙面积。体内研究进一步表明,AGP3水凝胶提供了一个促进内源性神经发生而非胶质纤维化形成的生物相容性微环境,从而导致显著的功能恢复。RNA测序分析进一步表明,AGP3水凝胶通过细胞内钙信号级联显著调节神经发生相关基因的表达。总体而言,这种超分子策略制备的AGP3水凝胶可作为填充腔隙并模拟脊髓生理特性的理想生物材料用于脊髓损伤修复。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b31/8941182/59d513bac0e2/ga1.jpg

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