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Taxanes: the genetic toxicity of paclitaxel and docetaxel in somatic cells of Drosophila melanogaster

机译:紫杉烷类:紫杉醇和多西紫杉醇对果蝇果蝇体细胞的遗传毒性

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摘要

In this study, the taxanes, paclitaxel and docetaxel were investigated for genotoxicity in the wing spot test of Drosophila melanogaster. These relatively new drugs are used in cancer therapy and show great promise in the treatment of a variety of cancers. Their major cellular target is the α,β-tubulin dimer but, unlike other spindle poisons, they stabilize microtubules by a shift towards assembly, producing nonfunctional microtubule bundles. The Drosophila wing Somatic Mutation and Recombination Test (SMART) provides a rapid means to evaluate agents able to induce gene mutations and chromosome aberrations, as well as rearrangements related to mitotic recombination. We applied the standard version of SMART (with normal bioactivation) and a variant version with increased cytochrome P450-dependent biotransformation capacity. In the standard assay, docetaxel was found to be aneuploidogenic; this was effectively abolished by a high cytochrome P450-dependent detoxification capacity. This suggests, as previously reported, the involvement of this family of enzymes in the detoxification of docetaxel rather than in its activation. In contrast, paclitaxel was clearly non-genotoxic at the same (millimolar) concentrations as used for docetaxel in both crosses. The weak responsiveness of SMART assays to aneugenic compounds, the weaker ligand and assembly action of paclitaxel and the more rapid reversibility of the microtubules formed with this compound, may have caused the negative response observed in the present study
机译:在这项研究中,研究了紫杉烷,紫杉醇和多西紫杉醇在果蝇果蝇翼点试验中的遗传毒性。这些相对较新的药物用于癌症治疗,在治疗多种癌症方面显示出巨大的希望。它们的主要细胞靶标是α,β-微管蛋白二聚体,但与其他纺锤体毒素不同,它们通过向组装转变来稳定微管,产生无功能的微管束。果蝇翼体细胞突变和重组试验(SMART)提供了一种快速的方法,可以评估能够诱导基因突变和染色体畸变以及与有丝分裂重组相关的重排的药物。我们应用了标准版的SMART(具有正常的生物激活)和具有增加的细胞色素P450依赖性生物转化能力的变体版本。在标准测定中,多西紫杉醇被发现具有非整倍性。高细胞色素P450依赖的排毒能力有效地消除了这种情况。如先前报道的,这表明该酶家族参与多西紫杉醇的解毒而不是其活化。相比之下,紫杉醇在与两个十字架中用于多西紫杉醇相同的浓度(毫摩尔)下显然没有遗传毒性。 SMART分析对气生化合物的响应性较弱,紫杉醇的配体和组装作用较弱以及与该化合物形成的微管的可逆性较快,可能导致了本研究中观察到的阴性反应

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