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新型生物活性基序及其在用于神经干细胞分化和神经组织工程的功能化自组装肽中的应用。

New bioactive motifs and their use in functionalized self-assembling peptides for NSC differentiation and neural tissue engineering.

机构信息

Center for Nanomedicine and Tissue Engineering, A.O. Ospedale Niguarda Ca' Granda, Milan, 20162, Italy.

出版信息

Nanoscale. 2012 Apr 28;4(9):2946-57. doi: 10.1039/c2nr30220a. Epub 2012 Apr 4.

DOI:10.1039/c2nr30220a
PMID:22476090
Abstract

Developing functionalized biomaterials for enhancing transplanted cell engraftment in vivo and stimulating the regeneration of injured tissues requires a multi-disciplinary approach customized for the tissue to be regenerated. In particular, nervous tissue engineering may take a great advantage from the discovery of novel functional motifs fostering transplanted stem cell engraftment and nervous fiber regeneration. Using phage display technology we have discovered new peptide sequences that bind to murine neural stem cell (NSC)-derived neural precursor cells (NPCs), and promote their viability and differentiation in vitro when linked to LDLK12 self-assembling peptide (SAPeptide). We characterized the newly functionalized LDLK12 SAPeptides via atomic force microscopy, circular dichroism and rheology, obtaining nanostructured hydrogels that support human and murine NSC proliferation and differentiation in vitro. One functionalized SAPeptide (Ac-FAQ), showing the highest stem cell viability and neural differentiation in vitro, was finally tested in acute contusive spinal cord injury in rats, where it fostered nervous tissue regrowth and improved locomotor recovery. Interestingly, animals treated with the non-functionalized LDLK12 had an axon sprouting/regeneration intermediate between Ac-FAQ-treated animals and controls. These results suggest that hydrogels functionalized with phage-derived peptides may constitute promising biomimetic scaffolds for in vitro NSC differentiation, as well as regenerative therapy of the injured nervous system. Moreover, this multi-disciplinary approach can be used to customize SAPeptides for other specific tissue engineering applications.

摘要

为了增强体内移植细胞的植入和刺激受损组织的再生,需要开发功能化的生物材料,这需要针对要再生的组织进行定制的多学科方法。特别是,神经组织工程可能会从发现促进移植干细胞植入和神经纤维再生的新型功能基序中获得巨大优势。我们使用噬菌体展示技术发现了与小鼠神经干细胞(NSC)衍生的神经前体细胞(NPC)结合的新肽序列,并将其与 LDLK12 自组装肽(SAPeptide)连接时,可促进其在体外的活力和分化。我们通过原子力显微镜、圆二色性和流变学对新功能化的 LDLK12 SAPeptides 进行了表征,获得了支持人源和鼠源 NSC 在体外增殖和分化的纳米结构水凝胶。最后,对一种具有最高体外干细胞活力和神经分化的功能化 SAPeptide(Ac-FAQ)进行了急性挫伤性脊髓损伤大鼠模型的测试,结果表明它促进了神经组织的再生和运动功能的恢复。有趣的是,用非功能化的 LDLK12 处理的动物的轴突发芽/再生处于 Ac-FAQ 处理动物和对照组之间的中间状态。这些结果表明,用噬菌体衍生肽功能化的水凝胶可能构成具有前景的仿生支架,可用于体外 NSC 分化以及受损神经系统的再生治疗。此外,这种多学科方法可用于针对其他特定的组织工程应用来定制 SAPeptides。

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