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异基因干细胞移植治疗多发性骨髓瘤:2007年至2017年的系统评价和荟萃分析

Allogeneic stem-cell transplantation for multiple myeloma: a systematic review and meta-analysis from 2007 to 2017.

作者信息

Yin Xuejiao, Tang Liang, Fan Fengjuan, Jiang Qinyue, Sun Chunyan, Hu Yu

机构信息

1Institute of Hematology, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Jiefang Dadao, Wuhan, 430022 China.

2Collaborative Innovation Center of Hematology, Huazhong University of Science and Technology, Jiefang Dadao, Wuhan, 430022 China.

出版信息

Cancer Cell Int. 2018 Apr 23;18:62. doi: 10.1186/s12935-018-0553-8. eCollection 2018.

Abstract

BACKGROUND

Despite recent advances, multiple myeloma (MM) remains incurable. However, the appearance of allogeneic stem cell transplantation (allo-SCT) through graft-versus-myeloma effect provides a potential way to cure MM to some degree. This systematic review aimed to evaluate the outcome of patients receiving allo-SCT and identified a series of prognostic factors that may affect the outcome of allo-SCT.

PATIENTS/METHODS: We systematically searched PubMed, Embase, and the Cochrane Library from 2007.01.01 to 2017.05.03 using the keywords 'allogeneic' and 'myeloma'.

RESULTS

A total of 61 clinical trials involving 8698 adult patients were included. The pooled estimates (95% CI) for overall survival (OS) at 1, 2, 3 and 5 years were 70 (95% CI 56-84%), 62 (95% CI 53-71%), 52 (95% CI 44-61%), and 46 (95% CI 40-52%), respectively; for progression-free survival were 51 (95% CI 38-64%), 40 (95% CI 32-48%), 34 (95% CI 27-41%), and 27 (95% CI 23-31%), respectively; and for treatment-related mortality (TRM) were 18 (95% CI 14-21%), 21 (95% CI 17-25%), 20 (95% CI 13-26%), and 27 (95% CI 21-33%), respectively. Additionally, the pooled 100-day TRM was 12 (95% CI 5-18%). The incidences of grades II-IV acute graft-versus-host disease (GVHD) and chronic GVHD were 34 (95% CI 30-37%) and 51 (95% CI 46-56%), respectively. The incidences of relapse rate (RR) and death rate were 50 (95% CI 45-55%) and 51 (95% CI 45-57%), respectively. Importantly, disease progression was the most major cause of death (48%), followed by TRM (44%). The results failed to show an apparent benefit of allo-SCT for standard risk patients, compared with tandem auto-SCT. In contrast, all 14 trials in our study showed that patients with high cytogenetic risk after allo-SCT had similar OS and PFS compared to those with standard risk, suggesting that allo-SCT may overcome the adverse prognosis of high cytogenetic risk.

CONCLUSION

Due to the lack of consistent survival benefit, allo-SCT should not be considered as a standard of care for newly diagnosed and relapsed standard-risk MM patients. However, for patients with high-risk MM who have a poor long-term prognosis, allo-SCT may be a strong consideration in their initial course of therapy or in first relapse after chemotherapy, when the risk of disease progression may outweigh the transplant-related risks. A large number of prospective randomized controlled trials were needed to prove the benefits of these therapeutic options.

摘要

背景

尽管近年来取得了进展,但多发性骨髓瘤(MM)仍然无法治愈。然而,通过移植物抗骨髓瘤效应进行的异基因干细胞移植(allo-SCT)的出现,为在一定程度上治愈MM提供了一种潜在途径。本系统评价旨在评估接受allo-SCT患者的结局,并确定一系列可能影响allo-SCT结局的预后因素。

患者/方法:我们使用关键词“异基因”和“骨髓瘤”,于2007年1月1日至2017年5月3日在PubMed、Embase和Cochrane图书馆进行了系统检索。

结果

共纳入61项临床试验,涉及8698例成年患者。1年、2年、3年和5年总生存期(OS)的合并估计值(95%CI)分别为70(95%CI 56-84%)、62(95%CI 53-71%)、52(95%CI 44-61%)和46(95%CI 40-52%);无进展生存期分别为51(95%CI 38-64%)、40(95%CI 32-48%)、34(95%CI 27-41%)和27(95%CI 23-31%);治疗相关死亡率(TRM)分别为18(95%CI 14-21%)、21(95%CI 17-25%)、20(95%CI 13-26%)和27(95%CI 21-33%)。此外,100天合并TRM为12(95%CI 5-18%)。II-IV级急性移植物抗宿主病(GVHD)和慢性GVHD的发生率分别为34(95%CI 30-37%)和51(95%CI 46-56%)。复发率(RR)和死亡率分别为50(95%CI 45-55%)和51(95%CI 45-57%)。重要的是,疾病进展是最主要的死亡原因(48%),其次是TRM(44%)。结果显示,与串联自体SCT相比,allo-SCT对标准风险患者未显示出明显益处。相反,我们研究中的所有14项试验表明allo-SCT后细胞遗传学高危患者与标准风险患者的OS和PFS相似,这表明allo-SCT可能克服细胞遗传学高危的不良预后。

结论

由于缺乏一致的生存获益,allo-SCT不应被视为新诊断和复发的标准风险MM患者的护理标准。然而,对于长期预后较差的高危MM患者,在其初始治疗过程中或化疗后的首次复发时,当疾病进展风险可能超过移植相关风险时,allo-SCT可能是一个重要的考虑因素。需要大量前瞻性随机对照试验来证明这些治疗选择的益处。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8dfb/5913895/d71885ad5c55/12935_2018_553_Fig1_HTML.jpg

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