Anisotropic microtopography surface of chitosan scaffold regulating skin precursor-derived schwann cells towards repair phenotype promotes neural regeneration

IF 5.6 1区医学 Q1 MATERIALS SCIENCE, BIOMATERIALS

Regenerative Biomaterials Pub Date : 2024-01-24 DOI:10.1093/rb/rbae005

Meng Cong, Xia Wu, Ling-jie Zhu, Guo-hao Gu, Fei Ding, Gui-cai Li, Hai-yan Shi

{"title":"Anisotropic microtopography surface of chitosan scaffold regulating skin precursor-derived schwann cells towards repair phenotype promotes neural regeneration","authors":"Meng Cong, Xia Wu, Ling-jie Zhu, Guo-hao Gu, Fei Ding, Gui-cai Li, Hai-yan Shi","doi":"10.1093/rb/rbae005","DOIUrl":null,"url":null,"abstract":"For repairing peripheral nerve and spinal cord defects, biomaterial scaffold-based cell-therapy was emerged as an effective strategy, requiring the positive response of seed cells to biomaterial substrate and environment signals. Previous work highlighted that the imposed surface properties of scaffold could provide important guidance cues to adhered cells for polarization. However, the insufficiency of native Schwann cells and unclear cellular response mechanisms remained to be addressed. Given that, this study aimed to illuminate the micropatterned chitosan-film action on the rat skin precursor-derived Schwann cells (SKP-SCs). Chitosan-film with different ridge/groove size was fabricated and applied for the SKP-SCs induction. Results indicated that SKP-SCs cultured on 30 μm size microgroove surface showed better oriented alignment phenotype. Induced SKP-SCs presented similar genic phenotype as repair Schwann cells, increasing expression of c-Jun, neural cell adhesion molecule, and neurotrophic receptor p75. Moreover, SKP-SC-secretome was subjected to cytokine array GS67 assay, data indicated the regulation of paracrine phenotype, a panel of cytokines was verified up-regulated at secreted level and gene expression level in induced SKP-SCs. These up-regulated cytokines exhibit a series of promotive neural regeneration functions, including cell survival, cell migration, cell proliferation, angiogenesis, axon growth, and cellular organization etc through bioinformatics analysis. Furthermore, the effectively polarized SKP-SCs-sourced secretome, promoted the proliferation and migration capacity of the primarily cultured native rat Schwann cells, and augmented neurites growth of the cultured motoneurons, as well as boosted axonal regrowth of the axotomy-injured motoneurons. Taken together, SKP-SCs obtained pro-neuroregeneration phenotype in adaptive response to the anisotropic topography surface of chitosan-film, displayed the oriented parallel growth, the transition towards repair Schwann cell genic phenotype, and the enhanced paracrine effect on neural regeneration. This study provided novel insights into the potency of anisotropic microtopography surface to Schwann-like cells phenotype regulation, that facilitating to provide promising engineered cell-scaffold in neural injury therapies.","PeriodicalId":20929,"journal":{"name":"Regenerative Biomaterials","volume":"329 1","pages":""},"PeriodicalIF":5.6000,"publicationDate":"2024-01-24","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Regenerative Biomaterials","FirstCategoryId":"5","ListUrlMain":"https://doi.org/10.1093/rb/rbae005","RegionNum":1,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"MATERIALS SCIENCE, BIOMATERIALS","Score":null,"Total":0}

引用次数: 0

Abstract

For repairing peripheral nerve and spinal cord defects, biomaterial scaffold-based cell-therapy was emerged as an effective strategy, requiring the positive response of seed cells to biomaterial substrate and environment signals. Previous work highlighted that the imposed surface properties of scaffold could provide important guidance cues to adhered cells for polarization. However, the insufficiency of native Schwann cells and unclear cellular response mechanisms remained to be addressed. Given that, this study aimed to illuminate the micropatterned chitosan-film action on the rat skin precursor-derived Schwann cells (SKP-SCs). Chitosan-film with different ridge/groove size was fabricated and applied for the SKP-SCs induction. Results indicated that SKP-SCs cultured on 30 μm size microgroove surface showed better oriented alignment phenotype. Induced SKP-SCs presented similar genic phenotype as repair Schwann cells, increasing expression of c-Jun, neural cell adhesion molecule, and neurotrophic receptor p75. Moreover, SKP-SC-secretome was subjected to cytokine array GS67 assay, data indicated the regulation of paracrine phenotype, a panel of cytokines was verified up-regulated at secreted level and gene expression level in induced SKP-SCs. These up-regulated cytokines exhibit a series of promotive neural regeneration functions, including cell survival, cell migration, cell proliferation, angiogenesis, axon growth, and cellular organization etc through bioinformatics analysis. Furthermore, the effectively polarized SKP-SCs-sourced secretome, promoted the proliferation and migration capacity of the primarily cultured native rat Schwann cells, and augmented neurites growth of the cultured motoneurons, as well as boosted axonal regrowth of the axotomy-injured motoneurons. Taken together, SKP-SCs obtained pro-neuroregeneration phenotype in adaptive response to the anisotropic topography surface of chitosan-film, displayed the oriented parallel growth, the transition towards repair Schwann cell genic phenotype, and the enhanced paracrine effect on neural regeneration. This study provided novel insights into the potency of anisotropic microtopography surface to Schwann-like cells phenotype regulation, that facilitating to provide promising engineered cell-scaffold in neural injury therapies.

查看原文本刊更多论文

壳聚糖支架的各向异性微表层可调控皮肤前体衍生的许旺细胞，使其趋向修复表型，从而促进神经再生

为了修复周围神经和脊髓缺损，基于生物材料支架的细胞疗法成为一种有效的策略，它需要种子细胞对生物材料基底和环境信号做出积极反应。之前的研究强调，支架的表面特性可为粘附细胞的极化提供重要的引导线索。然而，原生许旺细胞的不足和不明确的细胞反应机制仍有待解决。有鉴于此，本研究旨在阐明微图案壳聚糖薄膜对大鼠皮肤前体衍生许旺细胞（SKP-SCs）的作用。研究人员制作了不同脊/槽尺寸的壳聚糖薄膜，并将其用于诱导SKP-SCs。结果表明，在 30 μm 大小的微凹槽表面培养的 SKP-SCs 表现出更好的定向排列表型。诱导的SKP-SCs表现出与修复的许旺细胞相似的基因表型，c-Jun、神经细胞粘附分子和神经营养受体p75的表达增加。此外，对SKP-SC分泌组进行了细胞因子阵列GS67检测，数据表明SKP-SC受到旁分泌表型的调控，一组细胞因子在诱导SKP-SC中的分泌水平和基因表达水平被上调。通过生物信息学分析，这些上调的细胞因子表现出一系列促进神经再生的功能，包括细胞存活、细胞迁移、细胞增殖、血管生成、轴突生长和细胞组织等。此外，SKP-SCs 源分泌组的有效极化，促进了主要培养的原生大鼠许旺细胞的增殖和迁移能力，增强了培养的运动神经元的神经元生长，并促进了轴突损伤的运动神经元的轴突生长。综上所述，SKP-SCs对壳聚糖薄膜各向异性地形表面的适应性反应获得了促进神经再生的表型，表现出定向平行生长、向修复许旺细胞基因表型过渡以及增强神经再生的旁分泌效应。这项研究为各向异性微形貌表面调控许旺样细胞表型的有效性提供了新的见解，有助于为神经损伤治疗提供有前景的工程细胞支架。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文求助全文

来源期刊

Regenerative Biomaterials Materials Science-Biomaterials

CiteScore

7.90

自引率

16.40%

发文量

审稿时长

10 weeks

期刊介绍： Regenerative Biomaterials is an international, interdisciplinary, peer-reviewed journal publishing the latest advances in biomaterials and regenerative medicine. The journal provides a forum for the publication of original research papers, reviews, clinical case reports, and commentaries on the topics relevant to the development of advanced regenerative biomaterials concerning novel regenerative technologies and therapeutic approaches for the regeneration and repair of damaged tissues and organs. The interactions of biomaterials with cells and tissue, especially with stem cells, will be of particular focus.