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Micronuclei induced by reverse transcriptase inhibitors in mononucleated and binucleated cells as assessed by the cytokinesis-block micronucleus assay

机译:通过细胞分裂阻滞微核试验评估逆转录酶抑制剂在单核和双核细胞中诱导的微核

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摘要

This study evaluated the clastogenic and/or aneugenic potential of three nucleoside reverse transcriptase inhibitors (zidovudine - AZT, lamivudine - 3TC and stavudine - d4T) using the cytokinesis-block micronucleus (CBMN) assay in human lymphocyte cultures. All three inhibitors produced a positive response when tested in binucleated cells. The genotoxicity of AZT and 3TC was restricted to binucleated cells since there was no significant increase in the frequency of micronuclei in mononucleated cells. This finding indicated that AZT and 3TC caused chromosomal breakage and that their genotoxicity was related to a clastogenic action. In addition to the positive response observed with d4T in binucleated cells, this drug also increased the frequency of micronuclei in mononucleated cells, indicating clastogenic and aneugenic actions. Since the structural differences between AZT and 3TC and AZT and d4T involve the 3' position in the 2'-deoxyribonucleoside and in an unsaturated 2',3',dideoxyribose, respectively, we suggest that an unsaturated 2', 3', dideoxyribose is responsible for the clastogenic and aneugenic actions of d4T.
机译:这项研究使用胞质分裂阻滞微核(CBMN)分析评估了人类淋巴细胞培养物中三种核苷逆转录酶抑制剂(齐多夫定-AZT,拉米夫定-3TC和司他夫定-d4T)的致胶质化和/或造血潜能。在双核细胞中测试时,所有三种抑制剂均产生阳性反应。 AZT和3TC的遗传毒性仅限于双核细胞,因为单核细胞中微核的频率没有显着增加。该发现表明AZT和3TC引起染色体断裂,并且它们的遗传毒性与杀乳作用有关。除了在双核细胞中观察到的d4T阳性反应外,该药还增加了单核细胞中微核的频率,表明产生了致胶质瘤作用和造血作用。由于AZT和3TC之间的结构差异以及AZT和d4T分别涉及2'-脱氧核糖核苷和不饱和2',3',二脱氧核糖的3'位置,因此我们建议不饱和2',3',二脱氧核糖为负责d4T的胶质生成和气生成作用。

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