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鉴定成年鼠骨髓中对促血小板生成素(TPO)有反应的祖细胞,这些祖细胞具有体内巨核细胞和红细胞生成潜能。

Characterization of thrombopoietin (TPO)-responsive progenitor cells in adult mouse bone marrow with in vivo megakaryocyte and erythroid potential.

机构信息

The Walter and Eliza Hall Institute of Medical Research, Parkville, Victoria 3052, Australia.

出版信息

Proc Natl Acad Sci U S A. 2012 Feb 14;109(7):2364-9. doi: 10.1073/pnas.1121385109. Epub 2012 Jan 30.

Abstract

Hematopoietic progenitor cells are the progeny of hematopoietic stem cells that coordinate the production of precise numbers of mature blood cells of diverse functional lineages. Identification of cell-surface antigen expression associated with hematopoietic lineage restriction has allowed prospective isolation of progenitor cells with defined hematopoietic potential. To clarify further the cellular origins of megakaryocyte commitment, we assessed the in vitro and in vivo megakaryocyte and platelet potential of defined progenitor populations in the adult mouse bone marrow. We show that megakaryocytes arise from CD150(+) bipotential progenitors that display both platelet- and erythrocyte-producing potential in vivo and that can develop from the Flt3(-) fraction of the pregranulocyte-macrophage population. We define a bipotential erythroid-megakaryocyte progenitor population, the CD150(+)CD9(lo)endoglin(lo) fraction of Lin(-)cKit(+)IL7 receptor alpha(-)FcγRII/III(lo)Sca1(-) cells, which contains the bulk of the megakaryocyte colony-forming capacity of the bone marrow, including bipotential megakaryocyte-erythroid colony-forming capacity, and can generate both erythrocytes and platelets efficiently in vivo. This fraction is distinct from the CD150(+)CD9(hi)endoglin(lo) fraction, which contains bipotential precursors with characteristics of increased megakaryocytic maturation, and the CD150(+)CD9(lo)endoglin(hi) fraction, which contains erythroid lineage-committed cells. Finally, we demonstrate that bipotential erythroid-megakaryocyte progenitor and CD150(+)CD9(hi)endoglin(lo) cells are TPO-responsive and that the latter population specifically expands in the recovery from thrombocytopenia induced by anti-platelet serum.

摘要

造血祖细胞是造血干细胞的后代,它们协调产生精确数量的成熟血液细胞,具有不同的功能谱系。鉴定与造血谱系限制相关的细胞表面抗原表达,使得能够前瞻性地分离具有明确造血潜能的祖细胞。为了进一步阐明巨核细胞分化的细胞起源,我们评估了成年小鼠骨髓中定义明确的祖细胞群体的体外和体内巨核细胞和血小板潜能。我们表明,巨核细胞来源于 CD150(+)双潜能祖细胞,这些祖细胞在体内具有血小板和红细胞生成潜能,并且可以从粒细胞-巨噬细胞前体的 Flt3(-)部分发育而来。我们定义了一个双潜能红系-巨核细胞祖细胞群体,即 Lin(-)cKit(+)IL7 受体 alpha(-)FcγRII/III(lo)Sca1(-)细胞中的 CD150(+)CD9(lo)endoglin(lo) 部分,该部分包含骨髓中巨核细胞集落形成能力的大部分,包括双潜能巨核细胞-红细胞集落形成能力,并且可以在体内有效地生成红细胞和血小板。该部分与 CD150(+)CD9(hi)endoglin(lo)部分不同,后者包含具有增加的巨核细胞成熟特征的双潜能前体,而 CD150(+)CD9(lo)endoglin(hi)部分包含红细胞谱系定向细胞。最后,我们证明了双潜能红系-巨核细胞祖细胞和 CD150(+)CD9(hi)endoglin(lo)细胞对 TPO 有反应,并且后一种群体在由抗血小板血清诱导的血小板减少症恢复中特异性扩增。

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