Department of Clinical Haematology, Oxford University Hospitals NHS Foundation Trust, Oxford, United Kingdom.
PH Associates, Marlow, United Kingdom.
PLoS One. 2020 Feb 21;15(2):e0229469. doi: 10.1371/journal.pone.0229469. eCollection 2020.
Treatment of transplant-ineligible (TNE) newly diagnosed multiple myeloma (NDMM) requires a balance between disease control and maintaining quality of life (QoL). Patients value treatment-free remission periods in this incurable condition, as they are associated with better QoL. We set out to study clinical outcomes of consecutive TNE NDMM patients in routine care treated in Thames Valley Cancer Network between 2009 and 2017. The primary outcome was the evaluation of the treatment-free interval (TFI) after 1st and subsequent lines of therapy in the total cohort and in individual subgroups, according to age (≤75 vs. >75 years), and co-morbidities using Charlson Co-morbidity Index (CCI): mild: 0-2 vs. moderate: 3-4 vs. severe: ≥5). Secondary outcomes include response rates, overall survival (OS) and progression-free survival (PFS) between subgroups: according to age and according to co-morbidities. In a total cohort of 292 patients, median TFI (IQR) was longest after first-line therapy 6.9 months (1.4-16.9), reducing after second line therapy to 1.8 months (.7-6.9), and after third line therapy to 0.6 months (0.2-1.5). Median TFI followed the same trend across the different subgroups, by age (≤75, >75 years) and by CCI (0-2, 3-4, ≥5). Overall response rate (ORR) to first line therapy for total cohort was 67%, with responses categorised as complete response (CR): 21%, very good partial response: 16%, partial response: 30%, stable disease: 18%, and progressive disease: 8%. ORR in individual subgroups by age were (≤75: 70% vs. >75: 63%), and by CCI (0-2: 65% vs. 3-4: 71% vs. ≥5: 77%). Median OS and PFS for the total cohort were (30.2 months, 95% CI: 23.8-36.9), and (9 months, 95% CI: 7.9-9.8), respectively. Patients aged >75 years showed a significant reduction in OS and PFS compared to those ≤75 years of age: OS (49.0 vs. 22.4 months, p<0.0001, HR: 2.08, 95% CI: 1.5-2.8), PFS (9.7 vs. 8.0 months, p<0.01, HR: 1.47, 95% CI: 1.1-1.9). Median OS was significantly reduced with worsening co-morbidities: (CCI 0-2: 52.4 months vs. CCI 3-4: 33.0 months vs. CCI ≥5: 24.0 months, p = 0.01, HR: 1.43, 95% CI: 1.1-1.9). Median PFS was significantly reduced in the severely co-morbid subgroup (CCI 0-2: 9.4 months vs. CCI 3-4: 9.6 months vs. CCI ≥5: 7.1 months, p = 0.025, HR: 1.3, 95% CI: 1.0-1.6). This study demonstrated that first line therapy in the TNE NDMM setting resulted in the longest TFI which was modest at a median of 6.9 months, and decreased significantly following subsequent lines of therapy and across the different subgroups by age and by co-morbidities. Therapy objective should be to maximise the benefit of first line treatment. We envisage that the recent shift towards a continuous therapeutic approach will benefit TNE patients in view of improved survival data demonstrated by a number phase 3 trials. When continuous therapy is not appropriate due to patient choice or toxicities, an efficacious (not limited to thalidomide and bortezomib) but tolerable first line FDT strategy, which can maximise TFI and maintain a good QoL, remains a reasonable alternative approach.
治疗不适合移植(TNE)的新发多发性骨髓瘤(NDMM)需要在疾病控制和维持生活质量(QoL)之间取得平衡。在这种无法治愈的情况下,患者重视无治疗缓解期,因为它们与更好的 QoL 相关。我们着手研究 2009 年至 2017 年期间在泰晤士河谷癌症网络中接受常规治疗的连续 TNE NDMM 患者的临床结果。主要结果是评估总队列和各个亚组中一线和二线治疗后的无治疗间隔(TFI),根据年龄(≤75 岁与>75 岁)和合并症使用 Charlson 合并症指数(CCI):轻度:0-2 与中度:3-4 与重度:≥5)。次要结果包括反应率、总生存期(OS)和无进展生存期(PFS)在亚组之间的差异:根据年龄和合并症。在 292 名患者的总队列中,一线治疗后的 TFI(IQR)最长,为 6.9 个月(1.4-16.9),二线治疗后降至 1.8 个月(0.7-6.9),三线治疗后降至 0.6 个月(0.2-1.5)。在不同的亚组中,TFI 遵循相同的趋势,包括年龄(≤75 岁、>75 岁)和 CCI(0-2、3-4、≥5)。一线治疗的总队列的总体反应率(ORR)为 67%,反应分为完全缓解(CR):21%,非常好的部分缓解:16%,部分缓解:30%,稳定疾病:18%,进展性疾病:8%。按年龄分层的亚组(≤75 岁:70% vs. >75 岁:63%)和 CCI(0-2:65% vs. 3-4:71% vs. ≥5:77%)的 ORR 情况。总队列的中位 OS 和 PFS 分别为(30.2 个月,95%CI:23.8-36.9)和(9 个月,95%CI:7.9-9.8)。>75 岁的患者与≤75 岁的患者相比,OS 和 PFS 显著降低:OS(49.0 与 22.4 个月,p<0.0001,HR:2.08,95%CI:1.5-2.8),PFS(9.7 与 8.0 个月,p<0.01,HR:1.47,95%CI:1.1-1.9)。随着合并症的恶化,中位 OS 显著降低:(CCI 0-2:52.4 个月与 CCI 3-4:33.0 个月与 CCI ≥5:24.0 个月,p = 0.01,HR:1.43,95%CI:1.1-1.9)。严重合并症亚组的中位 PFS 显著降低(CCI 0-2:9.4 个月与 CCI 3-4:9.6 个月与 CCI ≥5:7.1 个月,p = 0.025,HR:1.3,95%CI:1.0-1.6)。本研究表明,TNE NDMM 治疗一线治疗导致的 TFI 最长,中位数为 6.9 个月,且在二线治疗后和根据年龄和合并症的不同亚组中显著降低。治疗目标应该是最大限度地提高一线治疗的效益。我们预计,鉴于一些 3 期试验显示的生存数据改善,最近向连续治疗方法的转变将使 TNE 患者受益。当由于患者选择或毒性而不适合连续治疗时,一种有效的(不仅限于沙利度胺和硼替佐米)但可耐受的一线 FDT 策略仍然是一种合理的替代方法,它可以最大限度地延长 TFI 并保持良好的 QoL。
