Dang Stephen M, Gerecht-Nir Sharon, Chen Jinny, Itskovitz-Eldor Joseph, Zandstra Peter W
Institute of Biomaterials and Biomedical Engineering, Department of Chemical Engineering and Applied Chemistry, University of Toronto, Toronto, Ontario, Canada.
Stem Cells. 2004;22(3):275-82. doi: 10.1634/stemcells.22-3-275.
Embryonic stem (ES) cells are of significant interest as a renewable source of therapeutically useful cells. ES cell aggregation is important for both human and mouse embryoid body (EB) formation and the subsequent generation of ES cell derivatives. Aggregation between EBs (agglomeration), however, inhibits cell growth and differentiation in stirred or high-cell-density static cultures. We demonstrate that the agglomeration of two EBs is initiated by E-cadherin-mediated cell attachment and followed by active cell migration. We report the development of a technology capable of controlling cell-cell interactions in scalable culture by the mass encapsulation of ES cells in size-specified agarose capsules. When placed in stirred-suspension bioreactors, encapsulated ES cells can be used to produce scalable quantities of hematopoietic progenitor cells in a controlled environment.
胚胎干细胞(ES细胞)作为一种可再生的治疗性有用细胞来源,备受关注。ES细胞聚集对于人和小鼠胚状体(EB)的形成以及随后ES细胞衍生物的产生都很重要。然而,EB之间的聚集(结块)会抑制搅拌或高细胞密度静态培养中的细胞生长和分化。我们证明,两个EB的结块是由E-钙黏蛋白介导的细胞附着引发的,随后是活跃的细胞迁移。我们报告了一种技术的开发,该技术能够通过将ES细胞大规模封装在尺寸特定的琼脂糖胶囊中,在可扩展培养中控制细胞间相互作用。当置于搅拌悬浮生物反应器中时,封装的ES细胞可用于在受控环境中产生可扩展数量的造血祖细胞。