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Comparative chemogenomics to examine the mechanism of action of DNA-targeted platinum-acridine anticancer agents

机译:比较化学基因组学研究的DNa靶向铂 - 吖抗癌剂的作用机制

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摘要

Platinum-based drugs have been used to successfully treat diverse cancers for several decades. Cisplatin, the original compound of this class, cross-links DNA, resulting in cell cycle arrest and cell death via apoptosis. Cisplatin is effective against several tumor types, yet it exhibits toxic side effects and tumors often develop resistance. To mitigate these liabilities while maintaining potency, we generated a library of non-classical platinum-acridine hybrid agents and assessed their mechanisms of action using a validated genome-wide screening approach in Saccharomyces cerevisiae and in the distantly related yeast Schizosaccharomyces pombe. Chemogenomic profiles from both S. cerevisiae and S. pombe demonstrate that several of the platinum-acridines damage DNA differently than cisplatin based on their requirement for distinct modules of DNA repair.
机译:铂基药物已成功用于治疗多种癌症数十年。顺铂是此类的原始化合物,它使DNA交联,从而导致细胞周期停滞并通过凋亡导致细胞死亡。顺铂对多种类型的肿瘤有效,但是它显示出毒副作用,并且肿瘤经常会产生耐药性。为了减轻这些负担,同时保持效力,我们建立了一个非经典的铂-啶杂化剂库,并使用经过验证的全基因组筛选方法在酿酒酵母和远缘相关的酵母裂殖酵母中评估了它们的作用机理。来自酿酒酵母和粟酒裂殖酵母的化学基因组谱表明,基于它们对DNA修复的不同模块的需求,几种铂-啶与顺铂对DNA的损伤不同。

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