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Mitosis and apoptosis: how is the balance set?

机译:有丝分裂和细胞凋亡:如何平衡?

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Anti-mitotic agents are used extensively during cancer chemotherapy. These agents target microtubules and thus block mitotic progression by activating the spindle assembly checkpoint. Following a prolonged mitotic arrest, cells either die in mitosis via apoptosis, or exit mitosis without dividing and survive, a process known as slippage. What dictates the balance between these two fates is unclear, but recent advances highlight the importance of the pro-survival Bcl2 family, with Mcl1 degradation emerging as a key determinant of mitotic cell fate. Here we review these advances, with a view towards identifying how the balance between apoptosis and slippage can be tipped in favour of death. This in turn may open up new opportunities to sensitize cancer cells to anti-mitotic agents.
机译:抗有丝分裂剂在癌症化疗期间被广泛使用。这些药物靶向微管,因此通过激活纺锤体装配检查点来阻止有丝分裂进程。长时间的有丝分裂停滞后,细胞要么通过凋亡在有丝分裂中死亡,要么退出有丝分裂而不分裂并存活,这一过程称为滑脱。决定这两种命运之间平衡的原因尚不清楚,但最近的进展突出了生存前Bcl2家族的重要性,而Mcl1降解已成为有丝分裂细胞命运的关键决定因素。在这里,我们回顾这些进展,以期确定如何可以调动细胞凋亡和滑脱之间的平衡,以利于死亡。反过来,这可能会开辟新的机会,使癌细胞对抗有丝分裂剂敏感。

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