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体内正在进行复制的小鼠造血干细胞的分离及其功能特性

Isolation and functional properties of murine hematopoietic stem cells that are replicating in vivo.

作者信息

Goodell M A, Brose K, Paradis G, Conner A S, Mulligan R C

机构信息

Whitehead Institute for Biomedical Research, Massachusetts Institute of Technology, Cambridge 02142, USA.

出版信息

J Exp Med. 1996 Apr 1;183(4):1797-806. doi: 10.1084/jem.183.4.1797.

Abstract

Hematopoietic stem cells (HSC) are multipotent cells that reside in the bone marrow and replenish all adult hematopoietic lineages throughout the lifetime of the animal. While experimenting with staining of murine bone marrow cells with the vital dye, Hoechst 33342, we discovered that display of Hoechst fluorescence simultaneously at two emission wavelengths revealed a small and distinct subset of whole bone marrow cells that had phenotypic markers of multipotential HSC. These cells were shown in competitive repopulation experiments to contain the vast majority of HSC activity from murine bone marrow and to be enriched at least 1,000-fold for in vivo reconstitution activity. Further, these Hoechst-stained side population (SP) cells were shown to protect recipients from lethal irradiation at low cell doses, and to contribute to both lymphoid and myeloid lineages. The formation of the Hoechst SP profile was blocked when staining was performed in the presence of verapamil, indicating that the distinctly low staining pattern of the SP cells is due to a multidrug resistance protein (mdr) or mdr-like mediated efflux of the dye from HSC. The ability to block the Hoechst efflux activity also allowed us to use Hoechst to determine the DNA content of the SP cells. Between 1 and 3% of the HSC were shown to be in S-G2M. This also enabled the purification of the G0-G1 and S-G2M HSC had a reconstitution capacity equivalent to quiescent stem cells. These findings have implications for models of hematopoietic cell development and for the development of genetic therapies for diseases involving hematopoietic cells.

摘要

造血干细胞(HSC)是多能细胞,存在于骨髓中,并在动物的整个生命周期内补充所有成体造血谱系。在用活性染料Hoechst 33342对小鼠骨髓细胞进行染色的实验中,我们发现,在两个发射波长同时显示Hoechst荧光揭示了一小部分独特的全骨髓细胞亚群,这些细胞具有多能造血干细胞的表型标记。在竞争性再增殖实验中表明,这些细胞包含了来自小鼠骨髓的绝大多数造血干细胞活性,并且体内重建活性至少富集了1000倍。此外,这些经Hoechst染色的侧群(SP)细胞在低细胞剂量下能保护受体免受致死性辐射,并对淋巴系和髓系谱系都有贡献。当在维拉帕米存在的情况下进行染色时,Hoechst SP图谱的形成被阻断,这表明SP细胞明显低染色模式是由于多药耐药蛋白(mdr)或类似mdr介导的染料从造血干细胞流出所致。阻断Hoechst流出活性的能力也使我们能够使用Hoechst来确定SP细胞的DNA含量。结果显示,1%至3%的造血干细胞处于S-G2M期。这也使得能够纯化G0-G1期和S-G2M期的造血干细胞,其重建能力与静止干细胞相当。这些发现对造血细胞发育模型以及涉及造血细胞疾病的基因治疗的发展具有重要意义。

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