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白细胞介素-3和利巴韦林在长期治疗巨核细胞白血病细胞系过程中诱导巨核细胞标志物和信息的高水平表达。

IL-3 and ribavirin induce high level expression of megakaryocytic markers and messages during long-term treatment of a megakaryocytic leukemia cell line.

作者信息

Majumdar A, Kerby S, Stenberg P E, Mullikin B, Beckstead J H, Cooney D A, Seidman M M

机构信息

Otsuka Pharmaceuticals, Rockville, Maryland 20850.

出版信息

J Cell Physiol. 1994 Jul;160(1):29-39. doi: 10.1002/jcp.1041600105.

DOI:10.1002/jcp.1041600105
PMID:8021297
Abstract

Megakaryocyte differentiation is a lengthy process with cells moving through a continuum delineated by the sequential expression of specific gene products. The limited number of primary cells available from marrow for analysis has brought attention to some leukemic cell lines which show enhanced megakaryocyte marker expression following incubation with inducing agents, the most common of which is phorbol myristate acetate (PMA). We developed an alternative induction protocol for the megakaryocytic leukemic cell line CMK, which involved incubation of the cells with IL-3 and the nucleoside analog, ribavirin, for 1-2 weeks. This treatment was neither toxic nor cytostatic and yielded increased levels of the surface glycoproteins GPIIb/IIIA and GPIb-IX. Levels of some megakaryocytic messages (GPIIIa, GPIX) showed a marked rise by 12 days of incubation in the inducer combination. This was due to a synergistic interaction between IL-3 and ribavirin which influenced both transcriptional and posttranscriptional events. Light and electron microscopy demonstrated the presence of large polyploid cells, with morphological features similar to those of megakaryocytes, in the induced cultures. Analysis of the heterogeneity of response in the cell population to the induction regimen after several days of treatment suggested that cells which failed to display surface markers had been stimulated by the inducers but did not have sufficient time to complete expression of that marker. The results were consistent with the view that the cells in the starting population were distributed along a temporal expression pathway, and those which were first to express the earliest marker would also lead in the expression of a later marker. The order of expression was the same as that during normal megakaryocyte development.

摘要

巨核细胞分化是一个漫长的过程,细胞会经历一系列由特定基因产物顺序表达所界定的连续阶段。由于可用于分析的骨髓原代细胞数量有限,一些白血病细胞系受到了关注,这些细胞系在与诱导剂孵育后会增强巨核细胞标志物的表达,其中最常见的诱导剂是佛波酯肉豆蔻酸乙酸酯(PMA)。我们为巨核细胞白血病细胞系CMK开发了一种替代诱导方案,该方案是将细胞与白细胞介素-3(IL-3)和核苷类似物利巴韦林孵育1至2周。这种处理既无毒性也不具有细胞抑制作用,并且使表面糖蛋白GPIIb/IIIA和GPIb-IX的水平升高。在诱导剂组合中孵育12天时,一些巨核细胞相关信息(GPIIIa、GPIX)的水平显著升高。这是由于IL-3和利巴韦林之间的协同相互作用,这种相互作用影响了转录和转录后事件。光镜和电镜检查显示,在诱导培养物中存在大的多倍体细胞,其形态特征与巨核细胞相似。对处理几天后细胞群体对诱导方案反应的异质性分析表明,未能显示表面标志物的细胞已受到诱导剂刺激,但没有足够时间完成该标志物的表达。结果与以下观点一致,即起始群体中的细胞沿着时间表达途径分布,那些最先表达最早标志物的细胞也将率先表达后期标志物。表达顺序与正常巨核细胞发育过程中的顺序相同。

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