Topoisomerase II (TOP2)-targeting anticancer chemotherapeutic drugs, termed TOP2 poisons, are widely used and effective in the clinic by stabilizing TOP2-DNA covalent complexes to induce DNA double-strand breaks (DSBs) and ultimately, cause cell death. The stabilized TOP2-DNA complex is known to be degraded by proteasome, whereas the underlying mechanism for instant TOP2β degradation in response to TOP2 poisons and the subsequent biological consequence remain elusive. Here, we reported that TOP2 poison-induced TOP2β degradation is mediated by SCFβ-TrCP ubiquitin ligase. Specifically, DNA damage signal, triggered by teniposide (VM-26) treatment, activates ATM, cooperating with CK1 to phosphorylate TOP2β on Ser1134 and Ser1130, respectively, in a canonical degron motif to facilitate β-TrCP binding and subsequent degradation. Inactivation of ATM, CK1 or SCFβ-TrCP by small molecular inhibitors or genetic knockdown/knockout abrogates TOP2β degradation. Biologically, blockage of TOP2β degradation in combination with VM-26 treatment impairs DNA damage response and repair, leading to an accelerated cell death via apoptosis. Thus, it appears that TOP2β degradation is a cellular defensive mechanism to facilitate the exposure of DSBs to trigger DNA damage response and repair. Collectively, our findings reveal a new strategy to improve the efficacy of TOP2 poisons in combination with small-molecule inhibitors against TOP2β degradation.

译文

靶向拓扑异构酶II(TOP2)的抗癌化学治疗药物,称为TOP2毒物,通过稳定TOP2-DNA共价复合物诱导DNA双链断裂(DSB)并最终导致细胞死亡,在临床上得到了广泛使用和有效。已知稳定的TOP2-DNA复合物可被蛋白酶体降解,而响应TOP2毒物而引起的即时TOP2β降解的基本机制以及随后的生物学后果仍然难以捉摸。在这里,我们报道了TOP2毒物诱导的TOP2β降解是由SCFβ-TrCP泛素连接酶介导的。具体而言,由替尼泊苷(VM-26)处理触发的DNA损伤信号激活ATM,与CK1协同作用以规范化的德格伦基序磷酸化Ser1134和Ser1130上的TOP2β,以促进β-TrCP结合和随后的降解。小分子抑制剂使ATM,CK1或SCFβ-TrCP失活或基因敲除/敲除消除了TOP2β的降解。从生物学上讲,TOP2β降解的阻断与VM-26治疗相结合会损害DNA损伤反应和修复,从而导致细胞通过凋亡加速死亡。因此,看来TOP2β降解是促进DSB暴露以触发DNA损伤反应和修复的细胞防御机制。总体而言,我们的发现揭示了一种新的策略,可与小分子抑制剂联合使用以提高TOP2毒物的功效,以对抗TOP2β降解。

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