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2-氯脱氧腺苷和苯丁酸氮芥对慢性淋巴细胞白血病的体外细胞毒性

In vitro cytotoxicity of 2-chlorodeoxyadenosine and chlorambucil in chronic lymphocytic leukemia.

作者信息

Begleiter A, Wang H, Verburg L, Lee K, Israels L G, Mowat M R, Johnston J B

机构信息

Manitoba Institute of Cell Biology, Manitoba Cancer Treatment and Research Foundation, Canada.

出版信息

Leukemia. 1996 Dec;10(12):1959-65.

PMID:8946937
Abstract

Chronic lymphocytic leukemia (CLL) is most commonly treated with the alkylating agent chlorambucil (CLB), although the nucleoside analogs, fludarabine (Flu) and 2-chlorodeoxyadenosine (CdA), are also effective in this disease. In this study, we investigated the in vitro cytotoxicity of CdA and CLB in CLL cells from 12 patients in vitro. Treatment with CLB for 6 h, followed by CdA for 18 h, resulted in 2.3- to 7.5-fold synergistic cytotoxicity in leukemic cells from 10 patients and an additive effect in cells from two patients. In general, synergy was greatest in patients who were sensitive to CLB or CdA, and could be enhanced by increasing the concentrations of CLB or CdA. Synergy was only observed if the cells were treated with CLB prior to CdA. Synergy could not be explained by an increase in the incorporation of CdA into DNA, or by the inhibition of repair of CLB-induced DNA crosslinks by CdA. In contrast to CLL cells, treatment of human marrow in vitro with CLB and CdA resulted in a low level of synergy for CFU-GM cells, and additive cell kill in erythroid progenitors. Thus, treatment with CdA and CLB can produce selective synergistic cell kill in CLL cells, and combination therapy may improve the therapeutic index of these agents in chemosensitive patients.

摘要

慢性淋巴细胞白血病(CLL)最常用烷化剂苯丁酸氮芥(CLB)进行治疗,尽管核苷类似物氟达拉滨(Flu)和2-氯脱氧腺苷(CdA)对这种疾病也有效。在本研究中,我们在体外研究了CdA和CLB对12例患者的CLL细胞的细胞毒性。先用CLB处理6小时,接着用CdA处理18小时,结果显示,10例患者的白血病细胞出现了2.3至7.5倍的协同细胞毒性,2例患者的细胞出现相加效应。一般来说,协同作用在对CLB或CdA敏感的患者中最为显著,并且可以通过增加CLB或CdA的浓度来增强。只有在细胞先用CLB处理后再用CdA处理时才观察到协同作用。协同作用无法用CdA掺入DNA的增加或CdA对CLB诱导的DNA交联修复的抑制来解释。与CLL细胞不同,体外使用CLB和CdA处理人骨髓时,CFU-GM细胞的协同作用水平较低,对红系祖细胞的细胞杀伤作用为相加效应。因此,用CdA和CLB进行治疗可在CLL细胞中产生选择性协同细胞杀伤作用,联合治疗可能会提高这些药物对化疗敏感患者的治疗指数。

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