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首页> 外文期刊>Journal of Translational Medicine >Updated survivals and prognostic factor analysis in myeloma treated by a staged approach use of bortezomib/thalidomide/dexamethasone in transplant eligible patients
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Updated survivals and prognostic factor analysis in myeloma treated by a staged approach use of bortezomib/thalidomide/dexamethasone in transplant eligible patients

机译:分阶段应用硼替佐米/沙利度胺/地塞米松治疗移植合格患者的骨髓瘤的更新生存率和预后因素分析

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Background Bortezomib, an NFkB inhibitor, is an active agent for the treatment of myeloma (MM). We have reported a promising complete remission (CR) rate for newly diagnosed myeloma patients treated by a staged approach, in which chemosensitive patients underwent autologous haematopoietic stem cell transplantation (auto-HSCT) while less chemosensitive patients received salvage therapy with bortezomib/thalidomide/dexamethasone prior to auto-HSCT. Methods Herein, with an additional 13 months of follow-up, we reported the updated survivals, and examined potential prognostic factors impacting event-free (EFS) and overall survival (OS). Results With a median follow-up of 30 months, the projected OS was 73% and EFS was 50.2%. Age, gender, clinical stage and DAPK methylation could not account for the differential chemosensitivity. Advanced ISS stage and DAPK methylation adversely impacted OS whereas oligoclonal reconstitution predicted superior EFS. Conclusions Our staged approach illustrated an economical use of expensive targeted agents while preserving a good CR rate and OS. The comparable survivals of chemosensitive and less chemosensitive patients suggested the staged approach might have abolished the adverse prognostic impact of suboptimal chemosensitivity. Finally, the adverse impact of DAPK methylation and favorable impact of oligoclonal reconstitution in myeloma warrants further study.
机译:背景硼替佐米是一种NFkB抑制剂,是用于治疗骨髓瘤(MM)的活性剂。我们已经报告了通过阶段性方法治疗的新诊断骨髓瘤患者的有希望的完全缓解(CR)率,其中对化学敏感性患者进行自体造血干细胞移植(auto-HSCT),对化学敏感性较差的患者则接受了硼替佐米/沙利度胺/地塞米松的挽救疗法在进行自动HSCT之前。方法在本文中,通过另外13个月的随访,我们报告了更新的生存率,并检查了影响无事件(EFS)和总体生存(OS)的潜在预后因素。结果平均随访30个月,预计OS为73%,EFS为50.2%。年龄,性别,临床分期和DAPK甲基化不能解释差异的化学敏感性。 ISS晚期和DAPK甲基化会对OS产生不利影响,而寡克隆重组可预测EFS更高。结论我们的分阶段方法说明了在保持良好的CR率和OS的同时经济地使用昂贵的靶向药物的方法。化学敏感性和化学敏感性较低的患者的可比生存率表明,分阶段的方法可能消除了化学敏感性不足的不良预后影响。最后,DAPK甲基化的不利影响和寡克隆重组对骨髓瘤的有利影响值得进一步研究。

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