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Applying macromolecular crowding to enhance extracellular matrix deposition and its remodeling in vitro for tissue engineering and cell-based therapies.

机译:施加大分子挤出以增强组织工程和细胞疗法体外细胞外基质沉积及其重塑。

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摘要

With the advent of multicellular organisms, the exterior of the cells evolved dramatically from highly aqueous surroundings into an extracellular matrix and space crowded with macromolecules. Cell-based therapies require removal of cells from their crowded physiological context and propagating them in dilute culture medium to attain therapeutically relevant numbers whilst preserving their phenotype. However, bereft of their microenvironment, cells under perform and lose functionality. Major efforts currently aim to modify cell culture surfaces and build three dimensional scaffolds to improve this situation. We discuss here alternative strategies that enable cells to re-create their own microenvironment in vitro, using carbohydrate-based macromolecules as culture media additives that create an excluded volume effect at defined fraction volume occupancies. This biophysical approach dramatically enhances extracellular matrix deposition by differentiated cells and stem cells, and boosts progenitor cell differentiation and proliferation. We begin to understand how well cells really can perform ex vivo if given the chance.
机译:随着多细胞生物的出现,细胞外部从高度含水环上从高度水性的周边进化到挤满大分子的细胞外基质和空间。基于细胞的疗法需要从其拥挤的生理背景中除去细胞并在稀释培养基中繁殖它们,以获得治疗其表型的治疗相关的数量。然而,他们的微环境,细胞正在进行和失去功能。目前旨在修改细胞培养表面并建立三维脚手架来改善这种情况的主要努力。我们在此讨论替代策略,使细胞能够在体外重新创建自己的微环境,使用基于碳水化合物的大分子作为培养介质添加剂,该添加剂在定义的分数占据占用培养介质添加剂。这种生物物理方法通过分化的细胞和干细胞显着增强细胞外基质沉积,并提高祖细胞分化和增殖。如果赋予机会,我们开始了解细胞真正可以执行exvivo的程度。

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