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具有 LN 和 BDNF 模拟表位的自组装肽水凝胶协同增强周围神经再生。

Self-assembling peptide hydrogels functionalized with LN- and BDNF- mimicking epitopes synergistically enhance peripheral nerve regeneration.

机构信息

State Key Laboratory of New Ceramics and Fine Processing, Key Laboratory of Advanced Materials of Ministry of Education, School of Materials Science and Engineering, Tsinghua University, Beijing 100084, China.

Institute of Orthopedics, Chinese PLA General Hospital, Beijing 100853, China; Co-innovation Center of Neuroregeneration, Nantong University, Nantong, Jiangsu Province 226007, China.

出版信息

Theranostics. 2020 Jul 9;10(18):8227-8249. doi: 10.7150/thno.44276. eCollection 2020.

Abstract

The regenerative capacity of the peripheral nervous system is closely related to the role that Schwann cells (SCs) play in construction of the basement membrane containing multiple extracellular matrix proteins and secretion of neurotrophic factors, including laminin (LN) and brain-derived neurotrophic factor (BDNF). Here, we developed a self-assembling peptide (SAP) nanofiber hydrogel based on self-assembling backbone Ac-(RADA)-NH (RAD) dual-functionalized with laminin-derived motif IKVAV (IKV) and a BDNF-mimetic peptide epitope RGIDKRHWNSQ (RGI) for peripheral nerve regeneration, with the hydrogel providing a three-dimensional (3D) microenvironment for SCs and neurites. Circular dichroism (CD), atomic force microscopy (AFM), and scanning electron microscopy (SEM) were used to characterize the secondary structures, microscopic structures, and morphologies of self-assembling nanofiber hydrogels. Then the SC adhesion, myelination and neurotrophin secretion were evaluated on the hydrogels. Finally, the SAP hydrogels were injected into hollow chitosan tubes to bridge a 10-mm-long sciatic nerve defect in rats, and gene expression at 1 week, axonal regeneration, target muscular re-innervation, and functional recovery at 12 weeks were assessed. The bioactive peptide motifs were covalently linked to the C-terminal of the self-assembling peptide and the functionalized peptides could form well-defined nanofibrous hydrogels capable of providing a 3D microenvironment similar to native extracellular matrix. SCs displayed improved cell adhesion on hydrogels with both IKV and RGI, accompanied by increased cell spreading and elongation relative to other groups. RSCs cultured on hydrogels with IKV and RGI showed enhanced gene expression of NGF, BDNF, CNTF, PMP22 and NRP2, and decreased gene expression of NCAM compared with those cultured on other three groups after a 7-day incubation. Additionally, the secretion of NGF, BDNF, and CNTF of RSCs was significantly improved on dual-functionalized peptide hydrogels after 3 days. At 1 week after implantation, the expressions of neurotrophin and myelin-related genes in the nerve grafts in SAP and Autograft groups were higher than that in Hollow group, and the expression of S100 in groups containing both IKV and RGI was significantly higher than that in groups containing either IKV or RGI hydrogels, suggesting enhanced SC proliferation. The morphometric parameters of the regenerated nerves, their electrophysiological performance, the innervated muscle weight and remodeling of muscle fibers, and motor function showed that RAD/IKV/RGI and RAD/IKV-GG-RGI hydrogels could markedly improve axonal regeneration with enhanced re-myelination and motor functional recovery through the synergetic effect of IKV and RGI functional motifs. We found that the dual-functionalized SAP hydrogels promoted RSC adhesion, myelination, and neurotrophin secretion and successfully bridged a 10-mm gap representing a sciatic nerve defect in rats . The results demonstrated the synergistic effect of IKVAV and RGI on axonal regrowth and function recovery after peripheral nerve injury.

摘要

周围神经系统的再生能力与施万细胞 (SCs) 在构建包含多种细胞外基质蛋白和神经营养因子的基底膜中的作用密切相关,这些神经营养因子包括层粘连蛋白 (LN) 和脑源性神经营养因子 (BDNF)。在这里,我们开发了一种基于自组装骨干 Ac-(RADA)-NH (RAD) 的自组装肽 (SAP) 纳米纤维水凝胶,该骨干 RAD 双重功能化了层粘连蛋白衍生的基序 IKVAV (IKV) 和 BDNF 模拟肽表位 RGIDKRHWNSQ (RGI),用于外周神经再生,水凝胶为 SC 和神经突提供了三维 (3D) 微环境。圆二色性 (CD)、原子力显微镜 (AFM) 和扫描电子显微镜 (SEM) 用于表征自组装纳米纤维水凝胶的二级结构、微观结构和形态。然后评估了水凝胶上的 SC 粘附、髓鞘形成和神经营养因子分泌。最后,将 SAP 水凝胶注入中空壳聚糖管中,以桥接大鼠 10mm 长的坐骨神经缺损,在第 1 周评估基因表达、轴突再生、靶肌肉再支配和功能恢复。生物活性肽基序通过共价键连接到自组装肽的 C 末端,功能化肽能够形成具有良好定义的纳米纤维水凝胶,能够提供类似于天然细胞外基质的 3D 微环境。与其他组相比,IKV 和 RGI 存在时,SCs 在水凝胶上显示出改善的细胞粘附,伴随着细胞铺展和伸长的增加。与其他三组相比,在培养 7 天后,在含有 IKV 和 RGI 的水凝胶上培养的 RSCs 表现出神经生长因子 (NGF)、BDNF、CNTF、PMP22 和 NRP2 的基因表达增加,而神经细胞黏附分子 (NCAM) 的基因表达降低。此外,在含有 IKV 和 RGI 的双功能化肽水凝胶上,SCs 的 NGF、BDNF 和 CNTF 分泌在 3 天后显著改善。植入后 1 周,SAP 和自体移植物组神经移植物中神经营养因子和髓鞘相关基因的表达高于空心组,而含有 IKV 和 RGI 的组中 S100 的表达明显高于仅含有 IKV 或 RGI 水凝胶的组,提示 SC 增殖增强。再生神经的形态学参数、电生理学性能、神经支配肌肉的重量和纤维重塑以及运动功能表明,RAD/IKV/RGI 和 RAD/IKV-GG-RGI 水凝胶通过 IKV 和 RGI 功能基序的协同作用,可显著改善轴突再生,增强髓鞘形成和运动功能恢复。我们发现,双功能化 SAP 水凝胶促进了 RSC 的粘附、髓鞘形成和神经营养因子的分泌,并成功桥接了代表大鼠坐骨神经缺损的 10mm 间隙。结果表明,IKVAV 和 RGI 对周围神经损伤后轴突的再生和功能恢复具有协同作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d94c/7381722/661bb1a84808/thnov10p8227g001.jpg

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