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首页> 外文期刊>Molecular cancer therapeutics >Microtubule dynamics, mitotic arrest, and apoptosis: drug-induced differential effects of betaIII-tubulin.
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Microtubule dynamics, mitotic arrest, and apoptosis: drug-induced differential effects of betaIII-tubulin.

机译:微管动力学,有丝分裂阻滞和凋亡:药物诱导的βIII-微管蛋白的差异作用。

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Overexpression of betaIII-tubulin is associated with resistance to tubulin-binding agents (TBA) in a range of tumor types. We previously showed that small interfering RNA silencing of betaIII-tubulin expression hypersensitized non-small cell lung cancer cells to TBAs. To determine whether betaIII-tubulin mediates its effect on drug-induced mitotic arrest and cell death by differentially regulating microtubule behavior, the effects of betaIII-tubulin knockdown on microtubule dynamics were analyzed in H460 non-small cell lung cancer cells stably expressing green fluorescent protein-betaI-tubulin. Interphase cells were examined at three vincristine and paclitaxel concentrations that (a) inhibited cell proliferation, (b) induced 5% to 10% mitotic arrest, and (c) induced 30% to 40% mitotic arrest. In the absence of either drug, betaIII-tubulin knockdown caused no significant change in microtubule dynamic instability. At 2 nmol/L vincristine (IC(50)), overall microtubule dynamicity was significantly suppressed in betaIII-tubulin knockdowns (-31.2%) compared with controls (-6.5%). Similar results were obtained with paclitaxel, suggesting that knockdown of betaIII-tubulin induces hypersensitivity by enhancing stabilization of microtubule dynamics at low drug concentrations. At higher drug concentrations (> or =40 nmol/L vincristine; > or =20 nmol/L paclitaxel), betaIII-tubulin knockdown resulted in significantly reduced suppressive effects on microtubule dynamicity with little or no further increase in mitotic arrest, compared with control cells. Importantly, apoptosis was markedly increased by betaIII-tubulin knockdown independent of further suppression of microtubule dynamics and mitotic arrest. These results show that betaIII-tubulin knockdown enhances the effectiveness of TBAs through two mechanisms: suppression of microtubule dynamics at low drug concentrations and a mitosis-independent mechanism of cell death at higher drug concentrations.
机译:βIII-微管蛋白的过表达与多种肿瘤类型对微管蛋白结合剂(TBA)的耐药性有关。我们以前表明,βIII-微管蛋白表达的小干扰RNA沉默会使非小细胞肺癌细胞对TBA过敏。为了确定βIII-微管蛋白是否通过差异调节微管行为来介导其对药物诱导的有丝分裂阻滞和细胞死亡的影响,在稳定表达绿色荧光蛋白的H460非小细胞肺癌细胞中分析了βIII-微管蛋白敲低对微管动力学的影响。 -βI-微管蛋白。在三个长春新碱和紫杉醇浓度下检查相间细胞,其中(a)抑制细胞增殖,(b)诱导5%至10%的有丝分裂停滞,和(c)诱导30%至40%的有丝分裂停滞。在没有任何一种药物的情况下,βIII-微管蛋白的敲低不会引起微管动态不稳定性的明显变化。在2 nmol / L长春新碱(IC(50))下,与对照组(-6.5%)相比,βIII-微管蛋白敲低(-31.2%)显着抑制了总体微管动力学。紫杉醇获得了相似的结果,表明敲低βIII-微管蛋白可通过增强低药物浓度下微管动力学的稳定性来诱导超敏反应。与对照组相比,在较高的药物浓度下(≥40 nmol / L长春新碱;≥20 nmol / L紫杉醇),βIII-微管蛋白的抑制作用导致对微管动力学的抑制作用显着降低,而有丝分裂阻滞作用几乎没有或没有进一步增加。细胞。重要的是,βIII-微管蛋白的敲低显着增加了细胞凋亡,而与进一步抑制微管动力学和有丝分裂阻滞无关。这些结果表明,βIII-微管蛋白的敲低通过两种机制增强了TBA的有效性:在低药物浓度下抑制微管动力学,在高药物浓度下有丝分裂独立的细胞死亡机制。

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