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• W2885455901 endingPage "377" @default.
• W2885455901 startingPage "361" @default.
• W2885455901 abstract "Aneuploidy is a hallmark of cancer. Defects in chromosome segregation result in aneuploidy. Multiple pathways are engaged in this process, including errors in kinetochore-microtubule attachments, supernumerary centrosomes, spindle assembly checkpoint (SAC) defects, and chromosome cohesion defects. Although aneuploidy provides an adaptation and proliferative advantage in affected cells, excessive aneuploidy beyond a critical level can be lethal to cancer cells. Given this, enhanced chromosome missegregation is hypothesized to limit survival of aneuploid cancer cells, especially when compared to diploid cells. Based on this concept, proteins and pathways engaged in chromosome segregation are being exploited as candidate therapeutic targets for aneuploid cancers. Agents that induce chromosome missegregation and aneuploidy now exist, including SAC inhibitors, those that alter centrosome fidelity and others that are under active study in preclinical and clinical contexts. This review explores the therapeutic potentials of such new agents, including the benefits of combining them with other antineoplastic agents." @default.
• W2885455901 created "2018-08-22" @default.
• W2885455901 creator A5083247969 @default.
• W2885455901 creator A5086058658 @default.
• W2885455901 creator A5091028729 @default.
• W2885455901 date "2019-01-06" @default.
• W2885455901 modified "2023-10-16" @default.
• W2885455901 title "New Cell Cycle Inhibitors Target Aneuploidy in Cancer Therapy" @default.
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