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Mitotic drug targets and the development of novel anti-mitotic anticancer drugs.

机译:有丝分裂药物靶点和新型抗丝体抗癌药物的发展。

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Drugs that interfere with the normal progression of mitosis belong to the most successful chemotherapeutic compounds currently used for anti-cancer treatment. Classically, these drugs are represented by microtubule binding drugs that inhibit the function of the mitotic spindle in order to halt the cell cycle in mitosis and to induce apoptosis in tumor cells. However, these compounds act not only on proliferating tumor cells, but exhibit significant side effects on non-proliferating cells including neurons that are highly dependent on intracellular transport processes mediated by microtubules. Therefore, there is a particular interest in developing novel anti-mitotic drugs that target non-microtubule structures. In fact, recently several novel drugs that target mitotic kinesins or the Aurora and polo-like kinases have been developed and are currently tested in clinical trials. In addition, approaches of cell cycle checkpoint abrogation during mitosis and at the G2/M transition inducing mitosis-associated tumor cell death are promising new strategies for anti-cancer therapy. It is expected that this "next generation" of anti-mitotic drugs will be as successful as the classical anti-microtubule drugs, while avoiding some of the adverse side effects.
机译:干扰有丝分裂正常进展的药物属于目前用于抗癌治疗的最成功的化学治疗化合物。经典上,这些药物由微管结合药物表示,所述微管粘合药物抑制有丝分裂主轴的功能,以使细胞周期停止有丝分裂并诱导肿瘤细胞中的细胞凋亡。然而,这些化合物不仅作用于增殖肿瘤细胞,而且表现出对不增殖细胞的显着副作用,包括高度依赖于由微管介导的细胞内传送过程的神经元。因此,对靶向非微管结构的新型抗丝体药物具有特别兴趣。实际上,最近已经开发了几种靶向有丝分裂性胰蛋白的新药或极光和鼠标碱基酶的新药,目前在临床试验中进行了测试。此外,细胞周期检查点消除在有丝分裂和G2 / m转变期间诱导有丝分裂相关的肿瘤细胞死亡的方法是对抗癌治疗的新策略。预计这一“下一代”的抗丝体药物将与古典抗微管药一样成功,同时避免了一些不良副作用。

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