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来自小鼠骨髓、动员外周血和胎肝的造血祖细胞的归巢和植入特性差异

Differential homing and engraftment properties of hematopoietic progenitor cells from murine bone marrow, mobilized peripheral blood, and fetal liver.

作者信息

Szilvassy S J, Meyerrose T E, Ragland P L, Grimes B

机构信息

Blood and Marrow Transplant Program, and the Division of Hematology/Oncology, Lucille P. Markey Cancer Center, University of Kentucky, Lexington, Kentucky 40536-0093, USA.

出版信息

Blood. 2001 Oct 1;98(7):2108-15. doi: 10.1182/blood.v98.7.2108.

Abstract

The rate of reconstitution following hematopoietic stem cell (HSC) transplantation differs widely depending on the tissue source of the cells infused. To test the hypothesis that variability in engraftment kinetics is related to differences in the efficiency with which intravenously transplanted HSCs "home" to the bone marrow (BM), the homing properties of murine fetal liver (FL), adult BM, and mobilized peripheral blood (MPB) cells were compared. Lethally irradiated mice transplanted with 2 x 10(6) FL, BM, or MPB cells exhibited sequentially slower recovery of circulating leukocytes and platelets that correlates with the progressively lower frequency of colony-forming cells (CFCs) in these tissues. However, differences in the rate and degree of early and long-term reconstitution were maintained even after infusing equal numbers of CFCs derived from FL, BM, and MPB. To compare the homing of progenitors from these tissues, cells were labeled with fluorescent PKH26 dye and injected into lethally irradiated hosts. Three hours later, PKH26(+) cells were reisolated from the BM and spleen by fluorescence-activated cell sorting and assayed for in vitro CFCs. Despite the higher level of very late antigen (VLA)-2, VLA-4, and VLA-5 on Sca-1(+)c-kit(+) cells from FL compared to BM, 10-fold fewer FL CFCs homed to hematopoietic organs than those from BM. MPB cells homed slightly better, but still less efficiently than BM cells. Therefore, clonogenic cells from different tissues exhibit striking variations in homing efficiency that does not necessarily correlate with engraftment kinetics. Homing is likely counterbalanced by intrinsic differences in proliferative potential that ultimately determine the rate of hematopoietic reconstitution.

摘要

造血干细胞(HSC)移植后的重建速率因输注细胞的组织来源不同而有很大差异。为了验证植入动力学的变异性与静脉移植的造血干细胞“归巢”至骨髓(BM)的效率差异相关这一假说,对小鼠胎肝(FL)、成年BM和动员外周血(MPB)细胞的归巢特性进行了比较。接受2×10⁶个FL、BM或MPB细胞移植的致死性照射小鼠,循环白细胞和血小板的恢复依次减慢,这与这些组织中集落形成细胞(CFC)频率的逐渐降低相关。然而,即使输注等量源自FL、BM和MPB的CFC后,早期和长期重建的速率及程度差异仍然存在。为了比较这些组织中祖细胞的归巢情况,用荧光PKH26染料标记细胞并注入致死性照射的宿主。3小时后,通过荧光激活细胞分选从BM和脾脏中重新分离出PKH26⁺细胞,并检测其体外CFC。尽管与BM相比,FL来源的Sca-1⁺c-kit⁺细胞上的极晚期抗原(VLA)-2、VLA-4和VLA-5水平更高,但归巢至造血器官的FL CFC比BM来源的少10倍。MPB细胞归巢稍好,但仍比BM细胞效率低。因此,来自不同组织的克隆形成细胞在归巢效率上表现出显著差异,这不一定与植入动力学相关。归巢可能被增殖潜能的内在差异所抵消,而增殖潜能最终决定造血重建的速率。

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