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Biomanufacturing of a chitosan/collagen scaffold to drive adhesion and alignment of human cardiomyocyte derived from stem cells

机译:壳聚糖/胶原屑支架的生物制造,以驱动源自干细胞的人心肌细胞的粘附和对准

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The in vitro generation of a three-dimensional (3D) myocardial tissue employing cells, biomaterials, and biomolecules is a promising strategy in cardiac tissue regeneration. Despite significant progresses in this field, cellular models are not yet able to provide a source of myocardial cells that will efficiently integrate and substitute damaged myocardial tissue. Stem cell-derived human cardiomyocytes (CMs) represent the most promising source for cardiac cell therapy. In order to sustain attachment, spreading, and orientation of human CMs on a scaffold we exploited an innovative negative replica patterning based on electrophoretic deposition to realize multi-scale micro-structured chitosan-collagen (C/C) scaffolds. Specific patterns were micro-structured on the cathode titanium disks using a laser machine. Cubic and hexagonal patterns were deeply characterized, and reproduced on the surface of the C/C scaffold. We initially challenged different blend with spontaneous contracting neonatal rat CMs to identificate the best substratum, finding that C/C 5:1 proportion can better sustain this type of culture. Finally, human CMs derived from induced pluripotent stem cells were seeded on these patterned scaffolds and colonization of the substrate was observed, thus confirming the validity of the chosen biomaterial. Moreover, preliminary experiments demonstrate the effectiveness of the pattern in controlling the orientation of human CMs. In conclusion, we designed and fabricated a scaffold that allows the attachment, spreading, and orientation of human CMs due to a correct C/C blend composition, to an innovative manufacturing process, and to an effective 3D architecture of the patterns. These data will surely help in solving the quest for a cardiac clinical patch.
机译:使用细胞,生物材料和生物分子的三维(3D)心肌组织的体外产生是心脏组织再生的有希望的策略。尽管该领域具有显着进展,但细胞模型尚未能够提供有效整合和替代受损的心肌组织的心肌细胞来源。干细胞衍生的人心肌细胞(CMS)代表心脏细胞疗法最有前途的来源。为了保持在支架附着,铺展,人类和CM的取向我们利用基于电泳沉积来实现多级微结构化壳聚糖 - 胶原(C / C)的支架一种创新的复制阴模图案化。使用激光机器在阴极钛盘上微结构的具体图案。立方体和六边形图案被深刻表征,并在C / C支架的表面上再现。我们最初挑战不同的混合物与自发的新生大鼠CMS识别最佳底层,发现C / C 5:1比例可以更好地维持这种类型的培养物。最后,将来自诱导多能干细胞的人CMS接种在这些图案化支架上,观察到基材的定植,从而证实了所选生物材料的有效性。此外,初步实验证明了模式控制人CMS取向的有效性。总之,我们设计和制造了一种脚手架,其允许由于正确的C / C混合组合物,创新制造过程以及模式的有效3D架构而导致人类CMS的连接,扩散和取向。这些数据肯定会有助于解决寻求心脏临床补丁。

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