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免疫固定电泳法检测完整 M 蛋白的骨髓瘤患者血清游离轻链:新型药物诱导治疗中反应评估和预后的潜在作用。

Serum free light chains in myeloma patients with an intact M protein by immunofixation: potential roles for response assessment and prognosis during induction therapy with novel agents.

机构信息

Department of Pharmacy, The Ohio State University Comprehensive Cancer Center, OH, USA.

出版信息

Hematol Oncol. 2012 Sep;30(3):156-62. doi: 10.1002/hon.1019. Epub 2011 Oct 26.

Abstract

The ascertainment of serum free light chain (sFLC) levels has been shown to be valuable in screening for the presence of plasma cell dyscrasia as well as for baseline prognosis in newly diagnosed patients. For patients with amyloidosis and those with oligo-secretory or non-secretory multiple myeloma (MM), serial measurement of sFLC has also been shown to be valuable in monitoring disease status. However, in patients with a measureable, intact monoclonal protein by immunofixation (M protein), the serial measurement of sFLC remains undefined and is currently not recommended in professional guidelines. Herein, we provide data comparing sFLC with M protein as biomarkers of response in newly diagnosed patients with MM undergoing induction therapy with the novel agents thalidomide, lenalidomide and/or bortezomib. We show that although M protein appears to outperform sFLC comparatively over the course of induction therapy, the addition of FLC to M protein further informs the characterization of residual disease status post-induction. Moreover, sFLC at the time of stem cell mobilization appears to hold prognostic power for survival endpoints following high-dose chemotherapy/autologous stem cell transplant (HDC/SCT). These findings suggest potentially novel roles for sFLC in patients with MM with an intact M protein receiving novel agent-based induction strategies followed by HDC/SCT.

摘要

血清游离轻链 (sFLC) 水平的测定已被证明在筛选浆细胞异常以及新诊断患者的基线预后方面具有价值。对于淀粉样变性患者以及寡分泌或非分泌性多发性骨髓瘤 (MM) 患者,sFLC 的连续测量也已被证明在监测疾病状态方面具有价值。然而,对于通过免疫固定 (M 蛋白) 可测量的完整单克隆蛋白的患者,sFLC 的连续测量仍然不明确,目前在专业指南中不推荐使用。在此,我们提供了比较 sFLC 与 M 蛋白作为新型药物沙利度胺、来那度胺和/或硼替佐米诱导治疗新诊断 MM 患者反应生物标志物的数据。我们表明,尽管在诱导治疗过程中 M 蛋白的表现似乎优于 sFLC,但在 M 蛋白中加入 FLC 可进一步说明诱导后残留疾病状态的特征。此外,干细胞动员时的 sFLC 似乎对接受新型药物诱导策略后进行高剂量化疗/自体干细胞移植 (HDC/SCT) 的生存终点具有预后能力。这些发现表明,对于接受新型药物诱导策略后进行 HDC/SCT 的完整 M 蛋白 MM 患者,sFLC 可能具有潜在的新作用。

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