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3-dimensional structures to enhance cell therapy and engineer contractile tissue

机译:3维结构,可增强细胞疗法并改造收缩组织

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Experimental studies in animals and recent human clinical trials have revealed the current limitations of cellular transplantation, which include poor cell survival, lack of cell engraftment, and poor differentiation. Evidence in animals suggests that use of a 3-dimensional scaffold may enhance cell therapy and engineer myocardial tissue by improving initial cell retention, survival, differentiation, and integration. Several scaffolds of synthetic or natural origin are under development. Until now, contractility has been demonstrated in vitro only in biological scaffolds prepared from decellularized organs or tissue, or in collagenic porous scaffold obtained by crosslinking collagen fibers. While contractility of a cellularized collagen construct is poor, it can be greatly enhanced by tumor basement membrane extract. Recent advances in biochemistry have shown improved cell-matrix interactions by coupling adhesionmolecules to achieve an efficient and safe bioartificial myocardium with no tumoral component. Fixation of adhesion molecules may also be a way to enhance cell homing and/or differentiation to increase local angiogenesis. Whatever the clinically successful combination ultimately proves to be, it is likely that cell therapy will require providing a supportive biochemical, physical, and spatial environment that will allow the cells to optimally differentiate and integrate within the target myocardial tissue.
机译:在动物中进行的实验研究和最近的人类临床试验已经揭示了细胞移植的当前局限性,包括细胞存活率低,缺乏细胞植入和分化差。动物方面的证据表明,使用三维支架可以改善初始细胞的保留,存活,分化和整合,从而增强细胞疗法并改造心肌组织。几种合成或天然来源的支架正在开发中。迄今为止,仅在体外由脱细胞器官或组织制备的生物支架中或在通过交联胶原纤维获得的胶原多孔支架中证明了可收缩性。虽然细胞化胶原蛋白构建体的收缩性较差,但可以通过肿瘤基底膜提取物大大增强其收缩性。生物化学方面的最新进展表明,通过偶联粘附分子可以实现有效而安全的无肿瘤成分的生物人工心肌,从而改善了细胞与基质之间的相互作用。粘附分子的固定也可以是增强细胞归巢和/或分化以增加局部血管生成的方式。无论临床上最终成功的组合是什么,细胞疗法可能都需要提供一种支持性的生化,物理和空间环境,使细胞能够最佳地分化并整合到目标心肌组织中。

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