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首页> 外文期刊>Russian Journal of Developmental Biology >Enhanced control of proliferation in telomerized cells
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Enhanced control of proliferation in telomerized cells

机译:增强对端粒细胞增殖的控制

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摘要

Clones of telomerized fibroblasts of adult human skin have earlier been obtained. It was shown that despite their fast growth in mass cultures, these cells poorly form colonies. Conditioned medium, antioxidants, and reduced partial oxygen pressure enhanced their colony formation, but not to the level characteristic of the initial cells. The conditioned medium of telomerized cells enhanced colony formation to a much greater extent than that of the initial cells. A study of proteome of the telomerized fibroblasts has revealed changes in the activities of tens of genes. A general trend consists in weakening and increased lability of the cytoskeleton and in activation of the mechanisms controlling protein degradation. However, these changes are not very pronounced. During the formation of immortal telomerized cells, selection takes place, which appears to determine changes in the expression of some genes. It was proposed that a decrease in the capacity of telomerized cells for colony formation is due to increased requirements of these cells to cell-cell contacts. The rate of cell growth reached that characteristic of mass cultures only in the largest colonies. In this respect, the telomerized fibroblasts resembled stem cells: they are capable of self-maintenance, but "escape" to differentiation in the absence of the corresponding microenvironment (niche), which is represented by other fibroblasts. Nondividing cells in the test of colony formation should be regarded as differentiated cells, since they have no features of degradation, preserve their viability, actively move, grow, phagocytize debris, etc. It was also shown that telomerization did not prevent differentiation of myoblasts and human neural stem cells. Thus, the results obtained suggest the existence of normal mechanisms underlying the regulation of proliferation in the telomerized cells, which opens possibilities of their use in cell therapy, especially in the case of autotransplantation to senior people, when the cell proliferative potential is markedly reduced and accessibility of stem cells is significantly restricted.
机译:成年人类皮肤的端粒化成纤维细胞的克隆已经较早获得。结果表明,尽管它们在大量培养物中快速生长,但它们很难形成菌落。条件培养基,抗氧化剂和降低的部分氧气压力可增强其菌落形成,但不能增强初始细胞的水平。端粒化细胞的条件培养基比初始细胞在更大程度上增强了集落形成。端粒化成纤维细胞的蛋白质组学研究揭示了数十种基因活性的变化。总的趋势在于细胞骨架的弱化和增加,以及控制蛋白质降解机制的激活。但是,这些变化不是很明显。在永生的端粒化细胞的形成过程中,发生选择,这似乎决定了某些基因表达的变化。有人提出端粒化细胞集落形成能力的降低是由于这些细胞对细胞-细胞接触的需求增加。细胞生长速率仅在最大的菌落中达到了大规模培养的特征。在这方面,端粒化的成纤维细胞类似于干细胞:它们能够自我维持,但是在没有相应的微环境(利基)的情况下“逃避”分化,而其他微纤维细胞则代表微环境。在集落形成测试中未分裂的细胞应被视为已分化的细胞,因为它们不具有降解特征,保持其生存力,活跃地移动,生长,吞噬碎片等。人类神经干细胞。因此,获得的结果表明存在端粒化细胞增殖调控的正常机制,这为细胞疗法的应用打开了可能性,特别是在向老年人自动移植的情况下,细胞增殖潜力显着降低并且干细胞的可及性受到极大限制。

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