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Use of cytometry technology for the study of stem cell biology

机译:细胞计数技术在干细胞生物学研究中的应用

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Hematopoietic stem cells (HSCs) are best-studied stem cells and they have contributed a great deal for the development of stem cell biology. HSCs reside in a bone marrow niche in a non-dividing state from which they occasionally are aroused to undergo cell division. Using highly purified HSCs by flow cytometry, we have recently shown that cytokine treatment of HSCs led to polarization of the lipid raft marker GM1 ganglioside as well as to phosphorylation of Akt and relocation of FOXO3a to the cytoplasm. Lipid raft clustering induced by cytokines is essential for HSC re-entry into the cell cycle. Furthermore, based on a hypothesis that signals from the niche inhibit LRC and induce hibernation in HSCs, we screened candidate niche signals for inhibition of LRC. Among niche signals examined, transforming growth factor-ß (TGF-ß) efficiently inhibits LRC and induces p57Kip2 expression, leading to HSC hibernation ex vivo. These data establish the role of TGF-ß as a niche signal in control of HSC hibernation and provide important clues to identify stem cell niche in bone marrow.
机译:造血干细胞(HSC)是研究最深入的干细胞,它们为干细胞生物学的发展做出了巨大贡献。 HSC处于非分裂状态的骨髓小生境中,偶尔会从中引起细胞分裂。通过流式细胞术使用高度纯化的HSC,我们最近显示,HSC的细胞因子处理导致脂质筏标记GM1神经节苷脂极化,以及Akt磷酸化和FOXO3a迁移至细胞质。细胞因子诱导的脂质筏聚集对于HSC重新进入细胞周期至关重要。此外,基于来自生态位的信号抑制LRC并诱导HSC休眠的假设,我们筛选了抑制LRC的候选生态位信号。在检查的利基信号中,转化生长因子-γ(TGF-β)有效抑制LRC并诱导p57 Kip2 表达,从而导致HSC体外冬眠。这些数据确立了TGF-β作为利基信号在控制HSC冬眠中的作用,并提供了重要的线索来鉴定骨髓中的干细胞利基。

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