Division of Hematology, Mayo Clinic, Rochester, Minnesota.
Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota.
Transplant Cell Ther. 2022 Nov;28(11):760.e1-760.e5. doi: 10.1016/j.jtct.2022.07.030. Epub 2022 Aug 5.
High-dose melphalan followed by autologous stem cell transplantation (ASCT) remains the standard of care for transplant-eligible patients with newly diagnosed multiple myeloma (NDMM). Achievement of complete response (CR) and minimal residual disease (MRD) negativity are associated with improved progression-free survival (PFS) and overall survival (OS). With superior triplet- and quadruplet-based induction regimens, a higher proportion of patients are achieving deep responses of at least a very good partial response (VGPR) or better. The probability of achieving different levels of deeper hematologic responses post-ASCT based on the pre-ASCT depth of response is less clear in the existing literature but would be of value to patients and providers in discussing the added benefit of ASCT. We assessed the rate of deepening the hematologic response with upfront ASCT in patients with NDMM, mainly to MRD-negative CR, based on the response achieved after induction therapy. We retrospectively reviewed 210 patients with NDMM who underwent upfront ASCT at Mayo Clinic Rochester between May 1, 2018, and July 31, 2019. In addition to the availability of next-generation flow cytometry (NGF) testing for MRD status, which yielded a sensitivity of 10, the more sensitive mass spectrometry-based assessment of peripheral blood (ie, MASS-FIX) for monoclonal proteins was used rather than conventional immunofixation. Pre-ASCT, 23 patients (11%) achieved MRD-negative CR, which increased to 66 patients (31%) post-ASCT. Of 187 patients not in MRD-negative CR pre-ASCT, 45 (24%) converted to MRD-negative CR. Patients with MRD-positive CR before ASCT had the highest rates of conversion to MRD-negative CR. HR cytogenetics did not impact rates of MRD-negative CR achievement post-ASCT irrespective of pre-ASCT IMWG response (P = 1.0). Overall, irrespective of IMWG response, 43 patients (20%) were MRD-negative pre-ASCT (19 in VGPR, 24 in CR or sCR), and 102 patients (49%) were MRD-negative post-ASCT (36 in VGPR, 66 in CR or sCR). Among 85 patients with VGPR post-ASCT, 36 achieved MRD negativity, of whom 8 (22%) progressed, whereas 49 had MRD-positive disease, of whom 24 (49%) progressed (P = .014). Upfront ASCT in patients with NDMM led to deeper responses, with 24% converting to MRD negative CR and more than doubling of the total rate of MRD negativity irrespective of IMWG response depth.
高剂量马法兰联合自体干细胞移植(ASCT)仍然是新诊断多发性骨髓瘤(NDMM)患者适合移植的标准治疗方法。完全缓解(CR)和微小残留病灶(MRD)阴性与无进展生存期(PFS)和总生存期(OS)的改善相关。由于采用了更高质量的三联和四联诱导方案,越来越多的患者达到了深度缓解,至少是非常好的部分缓解(VGPR)或更好。在现有文献中,基于 ASCT 前反应深度,接受 ASCT 后不同程度的血液学反应加深的概率尚不清楚,但对患者和提供者讨论 ASCT 的附加益处将具有重要价值。我们评估了在 Mayo 诊所罗彻斯特分校接受 ASCT 的 NDMM 患者在 ASCT 前加深血液学反应的概率,主要是达到 MRD 阴性 CR,基于诱导治疗后的反应。我们回顾性分析了 2018 年 5 月 1 日至 2019 年 7 月 31 日期间在 Mayo 诊所罗彻斯特分校接受 ASCT 的 210 名 NDMM 患者。除了可以使用下一代流式细胞术(NGF)检测 MRD 状态(灵敏度为 10)外,我们还使用了基于质谱的外周血更灵敏的评估方法(即 MASS-FIX)来检测单克隆蛋白,而不是常规免疫固定。在 ASCT 前,有 23 名(11%)患者达到了 MRD 阴性 CR,而在 ASCT 后,这一比例增加到了 66 名(31%)。在 ASCT 前未达到 MRD 阴性 CR 的 187 名患者中,有 45 名(24%)转为 MRD 阴性 CR。在 ASCT 前 MRD 阳性 CR 的患者中,转为 MRD 阴性 CR 的比例最高。HR 细胞遗传学对 ASCT 后 MRD 阴性 CR 发生率的影响与 IMWG 反应无关(P=1.0)。总体而言,无论 IMWG 反应如何,43 名(20%)患者在 ASCT 前为 MRD 阴性(19 名患者为 VGPR,24 名患者为 CR 或 sCR),102 名(49%)患者在 ASCT 后为 MRD 阴性(36 名患者为 VGPR,66 名患者为 CR 或 sCR)。在 85 名 ASCT 后达到 VGPR 的患者中,有 36 名达到了 MRD 阴性,其中 8 名(22%)进展,而 49 名患者有 MRD 阳性疾病,其中 24 名(49%)进展(P=0.014)。在 NDMM 患者中进行 ASCT 可导致更深的反应,24%的患者转为 MRD 阴性 CR,MRD 阴性的总发生率增加了一倍以上,而与 IMWG 反应深度无关。
