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首页> 外文期刊>Biology of blood and marrow transplantation: journal of the American Society for Blood and Marrow Transplantation >Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma
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Trends in utilization and outcomes of autologous transplantation as early therapy for multiple myeloma

机译:自体移植作为多发性骨髓瘤早期治疗的利用趋势和转归

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摘要

The impact of novel drugs for treating multiple myeloma (MM) on the utilization and outcomes of autologous hematopoietic progenitor cell transplantation (AHPCT) is unknown. We reviewed characteristics and outcomes of 20,278 patients who underwent AHPCT within 12months of diagnosis of MM in the United States and Canada and registered at the Center for International Blood and Marrow Transplant Research (CIBMTR) in 3 time cohorts reflecting the increasing availability of novel drugs: 1995 to 1999 (n=2226), 2000 to 2004 (n=6408), and 2005 to 2010 (n=11,644). In the United States, the number of AHPCTs performed increased at a greater rate than new MM cases. Patients in recent cohorts were older, less likely to have stage 3MM, and more likely to have received previous thalidomide, lenalidomide, or bortezomib. On multivariate analysis, AHPCT in the 2000 to 2004 cohort (HR=0.77) or in the 2005 to 2010 cohort (HR=0.68) were associated with lower risk of death. Survival at 60months post-AHPCT improved from 47% in 1995 to 1999 to 55% in 2000 to 2004 and to 57% in 2005 to 2010, owing less to improvement in progression-free survival (50% versus 55% versus 57% at 24months) than to postrelapse/progression survival (58% versus 65% versus 72% at 24months). AHPCT and new biological agents are complementary, nonredundant therapies and should be combined in the management of MM in suitable patients.
机译:未知治疗多发性骨髓瘤(MM)的新药对自体造血祖细胞移植(AHPCT)的利用和结果的影响。我们回顾了20278例在美国和加拿大诊断为MM的12个月内接受AHPCT并在国际血液和骨髓移植研究中心(CIBMTR)进行了3次研究的队列中登记的患者的特征和结果,这些研究反映了新药的日益普及: 1995年至1999年(n = 2226),2000年至2004年(n = 6408)和2005年至2010年(n = 11,644)。在美国,与新的MM案件相比,执行的AHPCT数量增加的幅度更大。最近队列中的患者年龄较大,进入3MM期的可能性较小,以前接受过沙利度胺,来那度胺或硼替佐米的可能性更高。在多变量分析中,AHPCT在2000年至2004年队列(HR = 0.77)或2005年至2010年队列(HR = 0.68)与较低的死亡风险相关。 AHPCT后60个月的生存率从1995年至1999年的47%提高到2000年至2004年的55%,以及2005年至2010年的57%,这归因于无进展生存率的提高(24个月时分别为50%,55%和57%) ),而不是复发/进展后存活率(24个月时分别为58%对65%对72%)。 AHPCT和新的生物制剂是互补的,非冗余的治疗方法,应在适合患者的MM管理中结合使用。

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