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粒细胞集落刺激因子在外周血祖细胞和干细胞动员及移植中的作用

The role of granulocyte colony-stimulating factor in mobilization and transplantation of peripheral blood progenitor and stem cells .

作者信息

Haas R, Murea S

机构信息

Department of Internal Medicine V, University of Heidelberg, Germany.

出版信息

Cytokines Mol Ther. 1995 Dec;1(4):249-70.

PMID:9384679
Abstract

The article provides a review of the role of granulocyte colony-stimulating factor (G-CSF) for mobilization and transplantation of peripheral blood progenitor and stem cells. Recombinant gene technology has permitted the production of highly purified material for therapeutic use in humans. Progenitor cells can be assessed using semisolid and liquid culture assays or direct immunofluorescence analysis of cells expressing CD34. This antigen is found on lineage-determined hematopoietic progenitor cells as well as on more primitive stem cells with extensive self-renewal capacity. Administration of G-CSF during steady-state hematopoiesis or following cytotoxic chemotherapy leads to an increase of hematopoietic progenitor cells in the peripheral blood. The level of circulating CD34+ cells post-chemotherapy is greater compared with G-CSF administration during steady state. On the other hand, CD34+ cells harvested post-chemotherapy contain a smaller proportion of more primitive progenitor cells (CD34+/HLA-DR- or CD34+/CD38-) compared with G-CSF treatment alone. Independent of the mobilization modality, the amount of previous cytotoxic chemo- and radiotherapy adversely affects the yield of hematopoietic progenitor cells. While continuous subcutaneous administration of G-CSF between 5 and 16 micrograms/kg bodyweight is preferred, additional dose-finding studies may be helpful to optimize current dose schedules. Adhesion molecules like L-selectin, VLA (very late antigen)-4 and LFA (leukocyte function antigen)-1 are likely to play a role in mobilization, since these antigens are expressed on CD34+ cells from bone marrow in different densities compared with blood-derived CD34+ cells collected following G-CSF-supported cytotoxic chemotherapy. It is also relevant for transplantation that during G-CSF-enhanced recovery post-chemotherapy, peripheral blood is enriched with a greater proportion of CD34+ cells expressing Thy-1 in comparison with CD34+ cells from bone marrow samples obtained on the same day or before the mobilization therapy was started. The early nature of the CD34+/Thy-1+ cells is very likely since this phenotype has been found on stem cells from human fetal liver and bone marrow and on cord blood cells. As a result, G-CSF-mobilized blood stem cells provide rapid and sustained engraftment following high-dose therapy, including myeloablative regimens. Positive selection of CD34+ cells as well as ex vivo expansion using different cytokines are currently being investigated for purging and improvement of short-term recovery post-transplantation. Future developments include the use of blood-derived hematopoietic stem cells for somatic gene therapy. The availability of growth factors has been an important prerequisite for the development of these new avenues for cell therapy.

摘要

本文综述了粒细胞集落刺激因子(G-CSF)在外周血祖细胞和干细胞动员及移植中的作用。重组基因技术已能生产出高度纯化的物质用于人类治疗。祖细胞可通过半固体和液体培养试验或对表达CD34的细胞进行直接免疫荧光分析来评估。这种抗原存在于谱系定向的造血祖细胞以及具有广泛自我更新能力的更原始干细胞上。在稳态造血期间或细胞毒性化疗后给予G-CSF会导致外周血中造血祖细胞增加。化疗后循环CD34+细胞的水平比稳态时给予G-CSF更高。另一方面,与单独使用G-CSF治疗相比,化疗后收获的CD34+细胞中更原始祖细胞(CD34+/HLA-DR-或CD34+/CD38-)的比例更小。无论动员方式如何,先前细胞毒性化疗和放疗的剂量都会对造血祖细胞的产量产生不利影响。虽然首选以5至16微克/千克体重连续皮下给予G-CSF,但额外的剂量探索研究可能有助于优化当前的剂量方案。像L-选择素、极迟抗原(VLA)-4和白细胞功能抗原(LFA)-1等黏附分子可能在动员中起作用,因为与G-CSF支持的细胞毒性化疗后收集的血源性CD34+细胞相比,这些抗原在骨髓CD34+细胞上的表达密度不同。同样与移植相关的是,在化疗后G-CSF增强恢复期间,与同一天或动员治疗开始前获得的骨髓样本中的CD34+细胞相比,外周血中表达Thy-1的CD34+细胞比例更高。CD34+/Thy-1+细胞很可能具有早期特性,因为这种表型已在人类胎儿肝脏和骨髓的干细胞以及脐带血细胞上发现。因此,G-CSF动员的血液干细胞在高剂量治疗(包括清髓方案)后能提供快速且持续的植入。目前正在研究对CD34+细胞进行阳性选择以及使用不同细胞因子进行体外扩增,以清除移植后细胞并改善短期恢复。未来的发展包括将血源性造血干细胞用于体细胞基因治疗。生长因子的可获得性是这些细胞治疗新途径发展的重要前提。

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