癌细胞利用核 Caspase-8 通过切割 USP28 来克服依赖 p53 的 G2/M 检查点。
Cancer Cells Employ Nuclear Caspase-8 to Overcome the p53-Dependent G2/M Checkpoint through Cleavage of USP28.
机构信息
Experimental Dermatology, Department of Dermatology, TU-Dresden, Dresden 01307, Germany; Center for Regenerative Therapies Dresden, TU-Dresden, Dresden 01307, Germany.
Experimental Dermatology, Department of Dermatology, TU-Dresden, Dresden 01307, Germany.
出版信息
Mol Cell. 2020 Mar 5;77(5):970-984.e7. doi: 10.1016/j.molcel.2019.12.023. Epub 2020 Jan 22.
Abstract
Cytosolic caspase-8 is a mediator of death receptor signaling. While caspase-8 expression is lost in some tumors, it is increased in others, indicating a conditional pro-survival function of caspase-8 in cancer. Here, we show that tumor cells employ DNA-damage-induced nuclear caspase-8 to override the p53-dependent G2/M cell-cycle checkpoint. Caspase-8 is upregulated and localized to the nucleus in multiple human cancers, correlating with treatment resistance and poor clinical outcome. Depletion of caspase-8 causes G2/M arrest, stabilization of p53, and induction of p53-dependent intrinsic apoptosis in tumor cells. In the nucleus, caspase-8 cleaves and inactivates the ubiquitin-specific peptidase 28 (USP28), preventing USP28 from de-ubiquitinating and stabilizing wild-type p53. This results in de facto p53 protein loss, switching cell fate from apoptosis toward mitosis. In summary, our work identifies a non-canonical role of caspase-8 exploited by cancer cells to override the p53-dependent G2/M cell-cycle checkpoint.
摘要
细胞质中的胱冬肽酶-8 是死亡受体信号的介质。虽然某些肿瘤中丢失了胱冬肽酶-8 的表达,但在其他肿瘤中却增加了,表明胱冬肽酶-8 在癌症中具有条件性的促生存功能。在这里,我们表明肿瘤细胞利用 DNA 损伤诱导的核胱冬肽酶-8 来绕过 p53 依赖性 G2/M 细胞周期检查点。在多种人类癌症中,胱冬肽酶-8 上调并定位于细胞核,与治疗耐药性和不良临床结局相关。胱冬肽酶-8 的耗竭会导致 G2/M 期 arrest、p53 的稳定以及肿瘤细胞中 p53 依赖性内在凋亡的诱导。在核内,胱冬肽酶-8 切割并失活泛素特异性肽酶 28(USP28),阻止 USP28 去泛素化并稳定野生型 p53。这导致事实上的 p53 蛋白丢失,将细胞命运从凋亡转向有丝分裂。总之,我们的工作确定了胱冬肽酶-8 被癌细胞利用的非典型作用,以绕过 p53 依赖性 G2/M 细胞周期检查点。
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