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锂与造血毒性。III. 单次给予环磷酰胺后体内造血功能的恢复

Lithium and hematopoietic toxicity. III. In vivo recovery of hematopoiesis following single-dose administration of cyclophosphamide.

作者信息

Gallicchio V S

机构信息

Department of Internal Medicine, University of Kentucky Medical Center, Lexington.

出版信息

Acta Haematol. 1988;79(4):192-7. doi: 10.1159/000205806.

Abstract

Studies are described that demonstrate the ability of lithium (Li) to enhance total peripheral blood neutrophil, platelet and stem cell (CFU-S, CFU-MIX, CFU-GM and CFU-MEG) populations from mice administered cyclophosphamide (CTX). Mice were preinjected on each of 3 consecutive days with ultrapure lithium carbonate (Li2CO3, 35 micrograms/kg b.w.) before receiving CTX (200 mg/kg, b.w.). Control groups were preinjected with phosphate-buffered saline (PBS) before receiving CTX. On days 1, 5, 7, 14, 21, and 28 following CTX, 3 mice from each group were sacrificed. Peripheral blood was obtained and examined for their packed red cell volume, white blood cell differential and platelet counts. Bone marrow and spleen cells were harvested and assayed for their stem cell content (CFU-S, CFU-MIX, CFU-GM, and CFU-MEG). Mice receiving Li prior to CTX did not develop thrombocytopenia and their absolute granulocyte counts recovered more rapidly when compared to CTX-PBS controls. Li-CTX bone marrow CFU-S and CFU-MIX were not as severely depressed when compared to the CTX-PBS controls. Li-CTX splenic-derived CFU-GM and CFU-MEG were increased significantly when compared to CTX-PBS controls and their rate of recovery was greater than that observed from bone marrow. These results demonstrate and confirm the capability of Li to accelerate hematopoietic recovery following the use of agents known to suppress hematopoiesis.

摘要

本文描述了多项研究,这些研究表明锂(Li)能够增强经环磷酰胺(CTX)处理的小鼠外周血中性粒细胞、血小板和干细胞(CFU-S、CFU-MIX、CFU-GM和CFU-MEG)的总数。在接受CTX(200mg/kg体重)之前,小鼠连续3天每天预先注射超纯碳酸锂(Li2CO3,35微克/千克体重)。对照组在接受CTX之前预先注射磷酸盐缓冲盐水(PBS)。在CTX处理后的第1、5、7、14、21和28天,每组处死3只小鼠。采集外周血,检测其红细胞压积、白细胞分类和血小板计数。收获骨髓和脾细胞,检测其干细胞含量(CFU-S、CFU-MIX、CFU-GM和CFU-MEG)。与CTX-PBS对照组相比,在CTX之前接受Li的小鼠未出现血小板减少,其绝对粒细胞计数恢复得更快。与CTX-PBS对照组相比,Li-CTX组的骨髓CFU-S和CFU-MIX没有受到同样严重的抑制。与CTX-PBS对照组相比,Li-CTX组脾脏来源的CFU-GM和CFU-MEG显著增加,并且其恢复速度比骨髓中观察到的更快。这些结果证明并确认了Li在使用已知抑制造血的药物后加速造血恢复的能力。

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