Morrison S J, Wright D E, Weissman I L
Department of Pathology, Stanford University, CA 94305, USA.
Proc Natl Acad Sci U S A. 1997 Mar 4;94(5):1908-13. doi: 10.1073/pnas.94.5.1908.
We isolated hematopoietic stem cells (HSC) from mice treated with cyclophosphamide (CY) and granulocyte colony-stimulating factor (G-CSF). All mobilized multipotent progenitor activity was contained in two populations: Thy-1(lo) Sca-1+ Lin- Mac-1- CD4- c-kit+ long-term reconstituting progenitors and Thy-1(lo) Sca-1+ Lin- Mac-1(lo) CD4- transiently reconstituting progenitors. CY/G-CSF treatment drove both long-term and transient multipotent progenitors into cycle, leading to a more than 12-fold expansion in the number of long-term self-renewing HSC prior to mobilization. After CY and 2 days of G-CSF treatment the number of bone marrow HSC began to decline and the number of blood and splenic HSC increased. HSC continued to proliferate in the bone marrow and spleen through 8 days of G-CSF treatment, but HSC released into the blood tended to be in G0/G1 phase. Mobilized multipotent progenitors isolated from the spleen were less efficient than normal bone marrow multipotent progenitors in engrafting irradiated mice but did not differ in colony forming unit-spleen (CFU-S) activity or single cell in vitro assays of primitive progenitor activity. The data suggest that mobilized HSC isolated from the spleen are less efficient at homing to and engrafting the bone marrow of irradiated recipient mice.
我们从接受环磷酰胺(CY)和粒细胞集落刺激因子(G-CSF)治疗的小鼠中分离出造血干细胞(HSC)。所有动员的多能祖细胞活性都包含在两个群体中:Thy-1(lo) Sca-1+ Lin- Mac-1- CD4- c-kit+长期重建祖细胞和Thy-1(lo) Sca-1+ Lin- Mac-1(lo) CD4-短暂重建祖细胞。CY/G-CSF治疗促使长期和短暂的多能祖细胞进入细胞周期,导致动员前长期自我更新的HSC数量增加了12倍以上。在CY和2天的G-CSF治疗后,骨髓HSC数量开始下降,而血液和脾脏HSC数量增加。在8天的G-CSF治疗期间,HSC在骨髓和脾脏中持续增殖,但释放到血液中的HSC倾向于处于G0/G1期。从脾脏中分离出的动员多能祖细胞在植入受辐照小鼠方面比正常骨髓多能祖细胞效率低,但在集落形成单位-脾脏(CFU-S)活性或原始祖细胞活性的单细胞体外测定中没有差异。数据表明,从脾脏中分离出的动员HSC在归巢和植入受辐照受体小鼠骨髓方面效率较低。
