Molecular Medicine Program and.
Division of Hematology, Oncology, and Blood and Marrow Transplantation, Department of Internal Medicine, University of Iowa, Iowa City, Iowa, USA.
J Clin Invest. 2018 Jul 2;128(7):2877-2893. doi: 10.1172/JCI98765. Epub 2018 Jun 4.
Drug resistance remains the key problem in cancer treatment. It is now accepted that each myeloma patient harbors multiple subclones and subclone dominance may change over time. The coexistence of multiple subclones with high or low chromosomal instability (CIN) signature causes heterogeneity and drug resistance with consequent disease relapse. In this study, using a tandem affinity purification-mass spectrometry (TAP-MS) technique, we found that NEK2, a CIN gene, was bound to the deubiquitinase USP7. Binding to USP7 prevented NEK2 ubiquitination resulting in NEK2 stabilization. Increased NEK2 kinase levels activated the canonical NF-κB signaling pathway through the PP1α/AKT axis. Newly diagnosed myeloma patients with activated NF-κB signaling through increased NEK2 activity had poorer event-free and overall survivals based on multiple independent clinical cohorts. We also found that NEK2 activated heparanase, a secreted enzyme, responsible for bone destruction in an NF-κB-dependent manner. Intriguingly, both NEK2 and USP7 inhibitors showed great efficacy in inhibiting myeloma cell growth and overcoming NEK2-induced and -acquired drug resistance in xenograft myeloma mouse models.
耐药性仍然是癌症治疗的关键问题。现在人们已经接受,每个骨髓瘤患者都存在多个亚克隆,并且亚克隆优势可能随时间而变化。具有高或低染色体不稳定性 (CIN) 特征的多个亚克隆的共存导致异质性和耐药性,从而导致疾病复发。在这项研究中,我们使用串联亲和纯化-质谱 (TAP-MS) 技术发现,CIN 基因 NEK2 与去泛素化酶 USP7 结合。与 USP7 的结合阻止了 NEK2 的泛素化,从而导致 NEK2 的稳定。增加的 NEK2 激酶水平通过 PP1α/AKT 轴激活了经典的 NF-κB 信号通路。根据多个独立的临床队列,新诊断的骨髓瘤患者中通过增加的 NEK2 活性激活 NF-κB 信号,其无事件生存和总生存较差。我们还发现,NEK2 以 NF-κB 依赖性方式激活了肝素酶,一种负责骨破坏的分泌酶。有趣的是,NEK2 和 USP7 抑制剂在抑制骨髓瘤细胞生长和克服异种移植骨髓瘤小鼠模型中由 NEK2 诱导和获得的耐药性方面均显示出很好的疗效。
