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核干细胞蛋白在细胞周期中持续表达,并在脂肪生成分化时下调,使其成为人类 MSC 增殖的重要标志物。

Continual expression throughout the cell cycle and downregulation upon adipogenic differentiation makes nucleostemin a vital human MSC proliferation marker.

机构信息

Department of Histology and Embryology, Ankara University School of Medicine, Sihhiye, 06100, Ankara, Turkey.

出版信息

Stem Cell Rev Rep. 2011 Jun;7(2):413-24. doi: 10.1007/s12015-010-9201-y.

DOI:10.1007/s12015-010-9201-y
PMID:21063916
Abstract

Nucleostemin (NS) is a nucleolar protein expressed in stem and cancer cells. In combination with nuclear/nucleolar proteins, NS has been demonstrated to be involved in cell-cycle regulation and telomere maintenance. NS expression reflects the cell's proliferation state indicating that the cell is active in the cell cycle, whereas NS signals disappear upon differentiation. This study analyzes the spatio-temporal (nucleolar/nuclear localization during interphase and M-phase) NS remodeling in two distinct human mesenchymal stem cell (MSC) populations to discriminate the NS differences, if any, throughout their stem cell and differentiation states. Beside its prominent multilobular nucleolar localization in interphase cells, coexistence of NS with chromosome arms during mitosis was also observed. Disruption of mitotic microtubules induced dissociation of NS from the chromosome arms and scattered it into the cytoplasm. Compared to deciduous dental pulp MSCs, NS mRNA expression gradually decreased upon aging in umbilical cord stroma-derived MSCs as culture time increased. Following adipogenic differentiation of the latter, NS signals gradually disappeared in both dividing and non-dividing cells, even before the morphological and functional signs of adipogenic transformation appeared. Quantitative NS mRNA measurements showed that MSCs from two sources exhibit a strong nucleostemin expression similar to embryonic stem cells. In conclusion, apart from its novel chromosomal localization shown in this study, nucleolar NS can be considered as a marker that indicates the proliferation/differentiation states in human MSCs. Moreover, differences in the relative NS protein and mRNA levels may reflect the degree of proliferation and can be used to characterize in vitro expansion capabilities.

摘要

核干细胞蛋白(NS)是一种在干细胞和癌细胞中表达的核仁蛋白。与核/核仁蛋白结合,NS 已被证明参与细胞周期调节和端粒维持。NS 表达反映了细胞的增殖状态,表明细胞在细胞周期中活跃,而在分化时 NS 信号消失。本研究分析了两种不同的人间充质干细胞(MSC)群体中 NS 的时空(间期和 M 期核仁/核定位)重塑,以区分其干细胞和分化状态下的 NS 差异(如果有)。除了在间期细胞中明显的多叶核仁定位外,还观察到 NS 与染色体臂在有丝分裂期间共存。有丝分裂微管的破坏诱导 NS 从染色体臂解离,并将其散布到细胞质中。与脱落乳牙牙髓 MSC 相比,随着培养时间的增加,脐带基质来源的 MSC 中 NS mRNA 表达逐渐降低。在后一种细胞向脂肪分化后,即使在出现脂肪生成转化的形态学和功能迹象之前,NS 信号在分裂和非分裂细胞中逐渐消失。定量 NS mRNA 测量表明,两种来源的 MSC 表现出强烈的核干细胞蛋白表达,类似于胚胎干细胞。总之,除了本研究中显示的其新颖的染色体定位外,核仁 NS 可被视为指示人 MSC 增殖/分化状态的标志物。此外,相对 NS 蛋白和 mRNA 水平的差异可能反映增殖程度,并可用于表征体外扩增能力。

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