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人类间充质干细胞衰老的不同方面。

Different facets of aging in human mesenchymal stem cells.

机构信息

Department of Stem Cell Biology and Cellular Engineering, Helmholtz-Institute for Biomedical Engineering, Aachen University Medical School, Aachen, Germany.

出版信息

Tissue Eng Part B Rev. 2010 Aug;16(4):445-53. doi: 10.1089/ten.TEB.2009.0825.

Abstract

Mesenchymal stem cells (MSCs) have to be culture expanded to gain relevant cell numbers for therapeutic applications. However, within 2-3 months the proliferation rate of MSCs decays until they ultimately reach a senescent state. This is accompanied by enlarged morphology, reduced expression of surface markers, and decreased differentiation potential. So far it is only scarcely understood how long-term culture affects MSC preparations, and five processes seem to be involved: (1) MSCs are composed of different sub-populations, and due to different proliferation rates the heterogeneity changes in the course of in vitro expansion; (2) cells in culture acquire mutations and other stochastic cellular defects; (3) self-renewal of MSCs may be impaired under culture conditions, leading to gradual differentiation; (4) the number of cell divisions might be restricted (e.g., by loss of telomeres), and (5) replicative senescence might be associated with the aging process of the organism. There is a growing perception that long-term culture has to be taken into account--especially for clinical applications. On the other hand, the state of replicative senescence is poorly defined by the number of population doublings or even by the number of passages. Reliable molecular measures for cellular aging are urgently needed.

摘要

间充质干细胞(MSCs)必须进行培养扩增,以获得用于治疗应用的相关细胞数量。然而,在 2-3 个月内,MSCs 的增殖速度会衰减,直到最终达到衰老状态。这伴随着形态增大、表面标志物表达减少和分化潜能降低。到目前为止,人们对长期培养如何影响 MSC 制剂知之甚少,似乎涉及五个过程:(1)MSCs 由不同的亚群组成,由于增殖速度不同,异质性在体外扩增过程中发生变化;(2)培养中的细胞获得突变和其他随机细胞缺陷;(3)MSC 的自我更新可能在培养条件下受损,导致逐渐分化;(4)细胞分裂的次数可能受到限制(例如,由于端粒丢失),以及(5)复制性衰老可能与生物体的衰老过程有关。人们越来越认识到,长期培养必须考虑在内--特别是对于临床应用。另一方面,复制性衰老的状态不能仅通过倍增次数甚至传代数来定义。迫切需要可靠的细胞衰老分子测量方法。

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