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2-氯-2'-阿拉伯糖基氟-2'-脱氧腺苷(氯法拉滨)与克拉屈滨对急性髓性白血病和慢性淋巴细胞白血病患者单核细胞细胞毒性的比较

Comparison of cytotoxicity of 2-chloro- 2'-arabino-fluoro-2'-deoxyadenosine (clofarabine) with cladribine in mononuclear cells from patients with acute myeloid and chronic lymphocytic leukemia.

作者信息

Lindemalm Synnöve, Liliemark Jan, Gruber Astrid, Eriksson Staffan, Karlsson Mats O, Wang Yuying, Albertioni Freidoun

机构信息

Department of Medicine, Division of Clinical Pharmacology, Karolinska Hospital, SE-171 76 Stockholm, Sweden.

出版信息

Haematologica. 2003 Mar;88(3):324-32.

PMID:12651272
Abstract

BACKGROUND AND OBJECTIVES

Clofarabine (CAFdA), one of the newer nucleoside drugs is undergoing a phase II clinical trial for the treatment of pediatric refractory/relapsed acute myeloid and lymphocytic leukemia. Although CAFdA is structurally similar to the clinically established analogs fludarabine and cladribine (CdA), its metabolism and mechanism of actions are significantly different. The present study investigates the in vitro cytotoxicity of CAFdA and CdA in mononuclear cells isolated from 52 patients with chronic lymphocytic (CLL) and acute myeloid leukemia (AML).

DESIGN AND METHODS

We incubated the leukemic cells with drugs for 48 hours and cytotoxicity was then evaluated by the MTT dye assay. We also determined the levels of deoxycytidine and deoxyguanosine kinase with radio-chemical substrate-based assays and used a high performance liquid chromatographic method to measure cellular nucleotides in leukemia cells after 2 hours' incubation.

RESULTS

Using equimolar concentrations of CAFdA and CdA, the in vitro cytotoxicity for the population was significantly higher with CAFdA than with CdA (median EC50 for CAFdA 0.12 microM and for CdA 0.15 microM, p<0.001). From the individual estimates the difference in cytotoxicity between CAFdA and CdA was more pronounced in cells from CLL patients (median EC50 for CAFdA 0.08 microM and for CdA 0.16 microM p<0.001) than in those from AML patients. We also found that CAFdA was phosphorylated more efficiently than CdA. No correlations were detected in this study between the levels of CdA and CAFdA nucleotides, enzymes levels and the in vitro responses.

INTERPRETATION AND CONCLUSIONS

The greater in vitro cytotoxicity and cell metabolism of CAFdA compared to CdA confirm the high activity of CAFdA and encourage clinical trials with CAFdA in leukemic patients.

摘要

背景与目的

氯法拉滨(CAFdA)是一种新型核苷类药物,正在进行治疗儿童难治性/复发性急性髓系和淋巴细胞白血病的II期临床试验。尽管CAFdA在结构上与临床已确立的类似物氟达拉滨和克拉屈滨(CdA)相似,但其代谢和作用机制却显著不同。本研究调查了CAFdA和CdA对52例慢性淋巴细胞白血病(CLL)和急性髓系白血病(AML)患者分离的单核细胞的体外细胞毒性。

设计与方法

我们将白血病细胞与药物孵育48小时,然后通过MTT染料法评估细胞毒性。我们还采用基于放射化学底物的测定法测定脱氧胞苷和脱氧鸟苷激酶的水平,并在孵育2小时后使用高效液相色谱法测量白血病细胞中的细胞核苷酸。

结果

使用等摩尔浓度的CAFdA和CdA,CAFdA对总体的体外细胞毒性显著高于CdA(CAFdA的中位EC50为0.12微摩尔,CdA为0.15微摩尔,p<0.001)。从个体评估来看,CAFdA和CdA之间的细胞毒性差异在CLL患者的细胞中(CAFdA的中位EC50为0.08微摩尔,CdA为0.16微摩尔,p<0.001)比在AML患者的细胞中更为明显。我们还发现CAFdA的磷酸化效率比CdA更高。在本研究中,未检测到CdA和CAFdA核苷酸水平、酶水平与体外反应之间的相关性。

解读与结论

与CdA相比,CAFdA具有更大的体外细胞毒性和细胞代谢,这证实了CAFdA的高活性,并鼓励在白血病患者中进行CAFdA的临床试验。

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