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New Bioengineering Insights into Human Neural Precursor Cell Expansion in Culture

机译:生物工程中人类神经前体细胞扩增的新见解

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Understanding initial cell growth, interactions associated with the process of expansion of human neural precursor cells (hNPCs), and cellular events pre- and postdifferentiation are important for developing bioprocessing protocols to reproducibly generate multipotent cells that can be used in basic research or the treatment of neurodegenerative disorders. Herein, we report the in vitro responses of telencephalon hNPCs grown in a serum-free growth medium using time-lapse live imaging as well as cell-surface marker, aggregate size, and immunocytochemical analyses. Time-lapse analysis of hNPC initial expansion indicated that cell-surface attachment in stationary culture and the frequency of cell-cell interaction in suspension conditions are important for subsequent aggregate formation and hNPC growth. In the absence of cell-surface attachment in low-attachment stationary culture, large aggregates of cells were formed and expansion was adversely affected. The majority of the telencephalon hNPCs expressed CD29, CD90, and CD44 (cell surface markers involved in cell-ECM and cell-cell interactions to regulate biological functions such as proliferation), suggesting that cell-surface attachment and cell-cell interactions play a significant role in the subsequent formation of cell aggregates and the expansion of hNPCs. Before differentiation, about 90% of the cells stained positive for nestin and expressed two neural precursor cells surface markers (CD 133 and CD24). Upon withdrawal of growth cytokines, hNPCs first underwent cell division and then differentiated preferentially towards a neuronal rather than a glial phenotype. This study provides key information regarding human NPC behavior under different culture conditions and favorable culture conditions that are important in establishing reproducible hNPC expansion protocols.
机译:了解初始细胞的生长,与人类神经前体细胞(hNPCs)的扩增过程相关的相互作用以及分化前和分化后的细胞事件对于开发可重复生成可用于基础研究或治疗的多能细胞的生物加工方案至关重要。神经退行性疾病。在这里,我们报告使用延时实时成像以及细胞表面标志物,聚集体大小和免疫细胞化学分析,在无血清生长培养基中生长的端脑hNPC的体外反应。 hNPC初始扩增的时移分析表明,固定培养中的细胞表面附着以及悬浮条件下细胞间相互作用的频率对于随后的聚集体形成和hNPC生长很重要。在低附着力固定培养中不存在细胞表面附着力时,会形成大的细胞聚集体,并且会对扩增产生不利影响。大多数端脑hNPCs表达CD29,CD90和CD44(参与细胞ECM和细胞间相互作用以调节生物学功能(例如增殖)的细胞表面标记),表明细胞表面附着和细胞间相互作用起着重要作用。在随后的细胞聚集体形成和hNPC扩增中发挥重要作用。在分化之前,约90%的细胞对Nestin染色呈阳性,并表达了两种神经前体细胞表面标记(CD 133和CD24)。在撤消生长细胞因子后,hNPC首先经历细胞分裂,然后优先向神经元而不是神经胶质表型分化。这项研究提供了有关在不同培养条件和有利培养条件下人类NPC行为的关键信息,这对于建立可重现的hNPC扩增方案至关重要。

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