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本文引用的文献

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Fractionation of an ECM hydrogel into structural and soluble components reveals distinctive roles in regulating macrophage behavior.将细胞外基质水凝胶分离为结构成分和可溶性成分,揭示了其在调节巨噬细胞行为中的独特作用。
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Biomaterial Approaches to Enhancing Neurorestoration after Spinal Cord Injury: Strategies for Overcoming Inherent Biological Obstacles.脊髓损伤后促进神经修复的生物材料方法:克服内在生物学障碍的策略
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Hydrogels and Cell Based Therapies in Spinal Cord Injury Regeneration.水凝胶与基于细胞的疗法在脊髓损伤再生中的应用
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Multifunctional therapeutic delivery strategies for effective neuro-regeneration following traumatic spinal cord injury.创伤性脊髓损伤后有效神经再生的多功能治疗递送策略
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Extracellular matrices, artificial neural scaffolds and the promise of neural regeneration.细胞外基质、人工神经支架与神经再生的前景
Neural Regen Res. 2014 Sep 1;9(17):1573-7. doi: 10.4103/1673-5374.141778.
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Clinical observation of umbilical cord mesenchymal stem cell transplantation in treatment for sequelae of thoracolumbar spinal cord injury.脐带间充质干细胞移植治疗胸腰段脊髓损伤后遗症的临床观察
J Transl Med. 2014 Sep 12;12:253. doi: 10.1186/s12967-014-0253-7.
7
Neurite-J: an image-J plug-in for axonal growth analysis in organotypic cultures.神经突-J:用于器官型培养中轴突生长分析的Image-J插件。
J Neurosci Methods. 2014 Oct 30;236:26-39. doi: 10.1016/j.jneumeth.2014.08.005. Epub 2014 Aug 12.
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The promotion of a constructive macrophage phenotype by solubilized extracellular matrix.可溶性细胞外基质促进建设性巨噬细胞表型。
Biomaterials. 2014 Oct;35(30):8605-12. doi: 10.1016/j.biomaterials.2014.06.060. Epub 2014 Jul 16.
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Spinal cord regeneration.脊髓再生
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10
Award winner for outstanding research in the PhD category, 2014 Society for Biomaterials annual meeting and exposition, Denver, Colorado, April 16-19, 2014: Decellularized adipose matrix hydrogels stimulate in vivo neovascularization and adipose formation.2014年生物材料学会年会暨展会博士类杰出研究奖获得者,科罗拉多州丹佛,2014年4月16日至19日:去细胞化脂肪基质水凝胶刺激体内新血管形成和脂肪生成。
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可注射细胞外基质水凝胶作为脊髓损伤修复的支架

Injectable Extracellular Matrix Hydrogels as Scaffolds for Spinal Cord Injury Repair.

作者信息

Tukmachev Dmitry, Forostyak Serhiy, Koci Zuzana, Zaviskova Kristyna, Vackova Irena, Vyborny Karel, Sandvig Ioanna, Sandvig Axel, Medberry Christopher J, Badylak Stephen F, Sykova Eva, Kubinova Sarka

机构信息

1 Institute of Experimental Medicine AS CR , Prague, Czech Republic .

2 2nd Medical Faculty, Charles University , Prague, Czech Republic .

出版信息

Tissue Eng Part A. 2016 Feb;22(3-4):306-17. doi: 10.1089/ten.TEA.2015.0422.

DOI:10.1089/ten.TEA.2015.0422
PMID:26729284
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4799710/
Abstract

Restoration of lost neuronal function after spinal cord injury (SCI) still remains a big challenge for current medicine. One important repair strategy is bridging the SCI lesion with a supportive and stimulatory milieu that would enable axonal rewiring. Injectable extracellular matrix (ECM)-derived hydrogels have been recently reported to have neurotrophic potential in vitro. In this study, we evaluated the presumed neuroregenerative properties of ECM hydrogels in vivo in the acute model of SCI. ECM hydrogels were prepared by decellularization of porcine spinal cord (SC) or porcine urinary bladder (UB), and injected into a spinal cord hemisection cavity. Histological analysis and real-time qPCR were performed at 2, 4, and 8 weeks postinjection. Both types of hydrogels integrated into the lesion and stimulated neovascularization and axonal ingrowth into the lesion. On the other hand, massive infiltration of macrophages into the lesion and rapid hydrogel degradation did not prevent cyst formation, which progressively developed over 8 weeks. No significant differences were found between SC-ECM and UB-ECM. Gene expression analysis revealed significant downregulation of genes related to immune response and inflammation in both hydrogel types at 2 weeks post SCI. A combination of human mesenchymal stem cells with SC-ECM did not further promote ingrowth of axons and blood vessels into the lesion, when compared with the SC-ECM hydrogel alone. In conclusion, both ECM hydrogels bridged the lesion cavity, modulated the innate immune response, and provided the benefit of a stimulatory substrate for in vivo neural tissue regeneration. However, fast hydrogel degradation might be a limiting factor for the use of native ECM hydrogels in the treatment of acute SCI.

摘要

脊髓损伤(SCI)后恢复丧失的神经元功能仍然是当前医学面临的一大挑战。一种重要的修复策略是用支持性和刺激性的环境来桥接脊髓损伤部位,以实现轴突重新布线。最近有报道称,可注射的细胞外基质(ECM)衍生水凝胶在体外具有神经营养潜力。在本研究中,我们在急性脊髓损伤模型中评估了ECM水凝胶在体内的假定神经再生特性。通过对猪脊髓(SC)或猪膀胱(UB)进行脱细胞处理制备ECM水凝胶,并将其注入脊髓半切腔。在注射后2周、4周和8周进行组织学分析和实时定量PCR。两种类型的水凝胶都融入损伤部位,刺激了新血管形成和轴突长入损伤部位。另一方面,巨噬细胞大量浸润到损伤部位以及水凝胶快速降解并不能阻止囊肿形成,囊肿在8周内逐渐发展。在脊髓ECM和膀胱ECM之间未发现显著差异。基因表达分析显示,在脊髓损伤后2周,两种水凝胶类型中与免疫反应和炎症相关的基因均显著下调。与单独使用脊髓ECM水凝胶相比,将人间充质干细胞与脊髓ECM联合使用并没有进一步促进轴突和血管长入损伤部位。总之,两种ECM水凝胶都桥接了损伤腔,调节了先天免疫反应,并为体内神经组织再生提供了刺激性基质的益处。然而,水凝胶的快速降解可能是天然ECM水凝胶用于治疗急性脊髓损伤的一个限制因素。