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重组人白细胞介素-7和重组人粒细胞集落刺激因子动员的祖细胞的数量及细胞周期差异

Quantitative and cell-cycle differences in progenitor cells mobilized by recombinant human interleukin-7 and recombinant human granulocyte colony-stimulating factor.

作者信息

Grzegorzewski K J, Komschlies K L, Franco J L, Ruscetti F W, Keller J R, Wiltrout R H

机构信息

Intramural Research Support Program, SAIC Frederick, MD, USA.

出版信息

Blood. 1996 Dec 1;88(11):4139-48.

PMID:8943848
Abstract

Administration of recombinant human interleukin-7 (rhIL-7) to mice increases the exportation of myeloid progenitors (colony-forming unit [CFU]-c and CFU-granulocyte erythroid megakaryocyte macrophage [CFU-GEMM]) from the bone marrow (BM) to peripheral organs, including blood, and also increases the number of primitive progenitor and stem cells in the peripheral blood (PB). We now report that combined treatment of mice with rhIL-7 and recombinant human granulocyte-colony stimulating factor (rhG-CSF) stimulates a twofold to 10-fold increase in the total number of PB CFU-c, and a twofold to fivefold increase in the total number of PB CFU-spleen at day 8 (CFU-S8) over the increase stimulated by rhIL-7 or rhG-CSF alone. In addition, the quality of mobilized cells with trilineage, long-term marrow-repopulating activity is maintained or increased in mice treated with rhIL-7 and rhG-CSF compared with rhIL-7 or rhG-CSF alone. These differences in mobilizing efficiency suggest qualitative differences in the mechanisms by which rhIL-7 and rhG-CSF mobilize progenitor cells, in fact, the functional status of progenitor cells mobilized by rhIL-7 differs from that of cells mobilized by rhG-CSF in that the incidence of actively cycling (S-phase) progenitors obtained from the PB is about 20-fold higher for rhIL-7-treated mice than for mice treated with rhG-CSF. These results suggest the use of rhIL-7-mobilized progenitor/stem cells for gene-modification and tracking studies, and highlight different functions and rates of repopulation after reconstitution with PB leukocytes obtained from mice treated with rhIL-7 versus rhG-CSF.

摘要

给小鼠注射重组人白细胞介素-7(rhIL-7)可增加骨髓(BM)中髓系祖细胞(集落形成单位[CFU]-c和CFU-粒系、红系、巨核系、巨噬系[CFU-GEMM])向外周器官(包括血液)的输出,还可增加外周血(PB)中原始祖细胞和干细胞的数量。我们现在报告,rhIL-7与重组人粒细胞集落刺激因子(rhG-CSF)联合治疗小鼠,在第8天可使PB CFU-c总数增加2至10倍,PB CFU-脾总数(CFU-S8)增加2至5倍,高于单独使用rhIL-7或rhG-CSF所刺激的增加量。此外,与单独使用rhIL-7或rhG-CSF相比,用rhIL-7和rhG-CSF治疗的小鼠中具有三系长期骨髓重建活性的动员细胞质量得以维持或提高。这些动员效率的差异表明rhIL-7和rhG-CSF动员祖细胞的机制存在质的差异,事实上,rhIL-7动员的祖细胞的功能状态与rhG-CSF动员的细胞不同,因为rhIL-7治疗的小鼠从PB获得的活跃循环(S期)祖细胞的发生率比rhG-CSF治疗的小鼠高约20倍。这些结果表明可将rhIL-7动员的祖细胞/干细胞用于基因修饰和追踪研究,并突出了用rhIL-7与rhG-CSF治疗的小鼠的PB白细胞重建后不同的功能和再填充率。

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