Mao Y, Desai S D, Ting C Y, Hwang J, Liu L F
Department of Pharmacology, University of Medicine and Dentistry of New Jersey-Robert Wood Johnson Medical School, Piscataway, New Jersey 08854-5635, USA.
J Biol Chem. 2001 Nov 2;276(44):40652-8. doi: 10.1074/jbc.M104009200. Epub 2001 Aug 23.
DNA topoisomerase II (TOP2) cleavable complexes represent an unusual type of DNA damage characterized by reversible TOP2-DNA cross-links and DNA double strand breaks. Many antitumor drugs and physiological stresses are known to induce TOP2 cleavable complexes leading to apoptotic cell death and genomic instability. However, the molecular mechanism(s) for repair of TOP2 cleavable complexes remains unclear. In the current studies, we show that TOP2 cleavable complexes induced by the prototypic TOP2 poison VM-26 are proteolytically degraded by the ubiquitin/26 S proteasome pathway. Surprisingly the TOP2beta isozyme is preferentially degraded over TOP2alpha isozyme. In addition, transcription inhibitors such as 5,6-dichlorobenzimidazole riboside and camptothecin can substantially block VM-26-induced TOP2beta degradation. These results are consistent with a model in which the repair of TOP2beta cleavable complexes may involve transcription-dependent proteolysis of TOP2beta to reveal the protein-concealed double strand breaks.
DNA拓扑异构酶II(TOP2)可切割复合物代表了一种特殊类型的DNA损伤,其特征为可逆的TOP2-DNA交联和DNA双链断裂。已知许多抗肿瘤药物和生理应激会诱导TOP2可切割复合物,导致凋亡性细胞死亡和基因组不稳定。然而,修复TOP2可切割复合物的分子机制仍不清楚。在当前的研究中,我们发现原型TOP2毒物VM-26诱导的TOP2可切割复合物通过泛素/26S蛋白酶体途径进行蛋白水解降解。令人惊讶的是,TOP2β同工酶比TOP2α同工酶更易被优先降解。此外,转录抑制剂如5,6-二氯苯并咪唑核糖核苷和喜树碱可显著阻断VM-26诱导的TOP2β降解。这些结果与一个模型相符,即TOP2β可切割复合物的修复可能涉及TOP2β的转录依赖性蛋白水解,以暴露蛋白质掩盖的双链断裂。
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