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首页> 外文期刊>European Journal of Haematology >Evaluation of the serum free light chain (sFLC) analysis in prediction of response in symptomatic multiple myeloma patients: rapid profound reduction in involved FLC predicts achievement of VGPR
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Evaluation of the serum free light chain (sFLC) analysis in prediction of response in symptomatic multiple myeloma patients: rapid profound reduction in involved FLC predicts achievement of VGPR

机译:评估血清游离轻链(sFLC)分析以预测有症状多发性骨髓瘤患者的反应:受累FLC的迅速大量减少可预测VGPR的实现

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Background: Observational data from clinical studies indicate that the goal of first-line therapy in newly diagnosed patients with symptomatic multiple myeloma (MM) should be very good partial response (VGPR) or better, preferably before high-dose treatment. We evaluated the value of early measurements of involved free light chains (iFLC) in prediction of high-quality responses. Measuring iFLC has a potential advantage due to a short half-life compared to the half-life of the M-protein. Methods: In 36 multiple myeloma (MM) patients, we measured serial changes in iFLC and M-protein after start of treatment. iFLC and M-protein were measured before treatment, the following 5 wk days, 2, 3 and 6 wks after start of treatment. Results: Median iFLC and M-protein half-life was 2.75 and 11.9 d, respectively. All patients with an iFLC >75 mg/L had an initial significant reduction (>20%) in iFLC, even patients with no response to treatment. The mean per cent reduction in iFLC 3 d after start of treatment was 52.3% and 23.6% (P= 0.021) in patients achieving >VGPR and PR, respectively. The mean per cent reduction in M-protein in patients achieving >VGPR and PR was not significantly different in the 6-wk study period. As a predictor of VGPR, an 80% reduction in iFLC at day 21 resulted in a sensitivity of 87.5% and a specificity of 100%. Conclusion: Changes in iFLC could be a tool for early identification of responders to anti-myeloma therapy. Early, sequential measurements of iFLC within the first week after start of treatment are not meaningful.
机译:背景:临床研究的观察数据表明,对新诊断的有症状多发性骨髓瘤(MM)患者进行一线治疗的目标应是非常好的局部缓解(VGPR)或更好,最好是在大剂量治疗之前。我们评估了涉及的游离轻链(iFLC)的早期测量对预测高质量响应的价值。与M蛋白的半衰期相比,测量iFLC具有半衰期短的潜在优势。方法:在36例多发性骨髓瘤(MM)患者中,我们测量了开始治疗后iFLC和M蛋白的系列变化。在治疗前,治疗后的第5周,第2、3和6周,测量iFLC和M蛋白。结果:中位iFLC和M蛋白半衰期分别为2.75和11.9 d。所有iFLC> 75 mg / L的患者,即使对治疗无反应的患者,iFLC的初始显着降低(> 20%)。开始治疗后3 d,达到> VGPR和PR的患者iFLC的平均减少分别为52.3%和23.6%(P = 0.021)。在6周的研究期内,达到> VGPR和PR的患者中M蛋白的平均减少百分比无显着差异。作为VGPR的预测指标,第21天iFLC降低80%时,灵敏度为87.5%,特异性为100%。结论:iFLC的改变可能是早期识别抗骨髓瘤治疗反应者的一种工具。在开始治疗后的第一周内,iFLC的早期顺序测量是没有意义的。

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