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Biofabrication Enables Efficient Interrogation and Optimization of Sequential Culture of Endothelial Cells, Fibroblasts, and Cardiomyocytes for Formation of Vascular Cords in Cardiac Tissue Engineering

机译:生物制造技术可以有效地询问和优化内皮细胞,成纤维细胞和心肌细胞的顺序培养,以形成心脏组织工程中的血管

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摘要

Biofabrication of living structures with desired topology and functionality requires the interdisciplinary effort of practitioners of the physical, life and engineering sciences. Such efforts are being undertaken in many laboratories around the world. Numerous approaches are pursued, such as those based on the use of natural or artificial scaffolds, decellularized cadaveric extracellular matrices and, most lately, bioprinting. To be successful in this endeavor, it is crucial to provide in vitro micro-environmental clues for the cells resembling those in the organism. Therefore, scaffolds, populated with differentiated cells or stem cells, of increasing complexity and sophistication are being fabricated. However, no matter how sophisticated scaffolds are, they can cause problems stemming from their degradation, eliciting immunogenic reactions and other a priori unforeseen complications. It is also being realized that ultimately the best approach might be to rely on the self-assembly and self-organizing properties of cells and tissues and the innate regenerative capability of the organism itself, not just simply prepare tissue and organ structures in vitro followed by their implantation. Here we briefly review the different strategies for the fabrication of three-dimensional biological structures, in particular bioprinting. We detail a fully biological, scaffoldless, print-based engineering approach that uses self-assembling multicellular units as bio-ink particles and employs early developmental morphogenetic principles, such as cell sorting and tissue fusion.
机译:具有所需拓扑结构和功能的生物结构的生物制造需要物理,生命和工程科学从业者的跨学科努力。全世界许多实验室都在进行这种努力。追求许多方法,例如基于使用天然或人工支架,脱细胞的尸体细胞外基质以及最近的生物印刷的方法。为了成功实现这一目标,至关重要的是为类似于生物体的细胞提供体外微环境线索。因此,正在制造由分化细胞或干细胞组成的,越来越复杂和复杂的支架。然而,无论多么复杂的支架,它们都可能由于其降解,引发免疫原性反应和其他先天未预见的并发症而引起问题。人们也意识到,最终最好的方法可能是依靠细胞和组织的自组装和自组织特性以及生物本身的固有再生能力,而不仅仅是在体外准备组织和器官结构,然后再进行体外培养。他们的植入。在这里,我们简要回顾了三维生物结构制造的不同策略,特别是生物印刷。我们详细介绍了一种完全生物学的,无支架的,基于印刷的工程方法,该方法使用自组装的多细胞单元作为生物墨水颗粒,并采用了早期的发育形态发生原理,例如细胞分选和组织融合。

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