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In pursuit of the allo-immune response in multiple myeloma: where do we go from here?

机译:为了追求多发性骨髓瘤的同种免疫反应:我们从这里去哪里?

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摘要

AlloSCT is a potentially curative procedure for haematological malignancies and marrow failure syndromes. However, unlike leukaemia and lymphoproliferative disorders, AlloSCT has yet to find its place in the clinical management of patients with multiple myeloma. AlloSCT in multiple myeloma is associated with a high procedure-related mortality (TRM up to 35%) when full-intensity conditioning is used and only up to 36% of cases show long-term disease-free survival. The introduction of reduced intensity conditioning AlloSCT, more recently following an autologous SCT, has reduced the TRM to <20%, but there is an associated increased relapse risk. The use of donor lymphocyte infusions and novel biological agents (thalidomide, bortezomib), alone or together, can be effective in relapsed and even persistent disease post-AlloSCT. Thus, in pursuit of the putative graft-versus-myeloma effect, we need to consider the whole patient management pathway both preceding (depth of response to novel agents) and post-AlloSCT, to minimize the toxicity while harnessing the adoptive immunotherapy effect. This review sets out what we have learned to date from the clinical research studies in this area, examines concepts for improving the outcomes of AlloSCT and proposes a potential direction of clinical investigation to maximize the effect of AlloSCT in multiple myeloma.
机译:AlloSCT是血液系统恶性肿瘤和骨髓衰竭综合征的潜在治疗方法。但是,与白血病和淋巴增生性疾病不同,AlloSCT尚未在多发性骨髓瘤患者的临床治疗中找到其位置。当使用全强度调理时,多发性骨髓瘤中的AlloSCT与手术相关的高死亡率(TRM高达35%)相关,只有高达36%的病例显示出长期无病生存。自体SCT后最近才引入强度降低的调理AlloSCT,已将TRM降低至<20%,但相关的复发风险增加。单独或一起使用供体淋巴细胞输注液和新型生物制剂(沙利度胺,硼替佐米)可​​有效治疗AlloSCT后复发甚至持续的疾病。因此,为了追求假定的移植物抗骨髓瘤的作用,我们需要考虑AlloSCT治疗之前(对新药的反应深度)和治疗后的整个患者管理途径,以最大程度地降低毒性,同时利用过继免疫疗法的作用。这篇综述阐述了我们从该领域的临床研究中学到的知识,探讨了改善AlloSCT结果的概念,并提出了临床研究的潜在方向,以最大化AlloSCT在多发性骨髓瘤中的作用。

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