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临床参数和诱导方案对多发性骨髓瘤患者外周血干细胞动员及采集的影响

Impact of Clinical Parameters and Induction Regimens on Peripheral Blood Stem-Cell Mobilization and Collection in Multiple Myeloma Patients.

作者信息

Sauer Sandra, Hieke Lennart, Brandt Juliane, Müller-Tidow Carsten, Schmitt Anita, Kauer Joseph, Kriegsmann Katharina

机构信息

Department of Hematology, Oncology and Rheumatology, University Hospital Heidelberg, Heidelberg, Germany.

Laborarztpraxis Rhein-Main MVZ GbR, Limbach Gruppe SE, Frankfurt am Main, Germany.

出版信息

Transfus Med Hemother. 2023 Jun 5;50(5):382-395. doi: 10.1159/000530056. eCollection 2023 Oct.

Abstract

INTRODUCTION

High-dose chemotherapy (HDCT) followed by autologous blood stem-cell transplantation (ABSCT) remains the standard consolidation therapy for newly diagnosed eligible multiple myeloma (MM) patients. As a prerequisite, peripheral blood stem cells (PBSCs) must be mobilized and collected by leukapheresis (LP). Many factors can hamper PBSC mobilization/collection. Here, we provide a comprehensive multiparametric assessment of PBSC mobilization/collection outcome parameters in a large cohort.

METHODS

In total, 790 MM patients (471 [60%] male, 319 [40%] female) who underwent PBSC mobilization/collection during first-line treatment were included. Evaluated PBSC mobilization/collection outcome parameters included the prolongation of PBSC mobilization, plerixafor administration, number of LP sessions, and overall PBSC collection goal/result.

RESULTS

741 (94%) patients received cyclophosphamide/adriamycin/dexamethasone (CAD) and granulocyte-colony-stimulating factor (G-CSF) mobilization. Plerixafor was administered in 80 (10%) patients. 489 (62%) patients started LP without delay. 530 (67%) patients reached the PBSC collection goal at the first LP session. The mean overall PBSC collection result was 10.3 (standard deviation [SD] 4.4) × 10 CD34 cells/kg. In a multiparametric analysis, variables negatively associated with PBSC mobilization/collection outcomes were female gender, age >60 years, an advanced ISS stage, and local radiation pre-/during induction, but not remission status postinduction. Notably, the identified risk factors contributed differently to each PBSC mobilization/collection outcome parameter. In this context, compared to all other induction regimens, lenalidomide-based induction with/without antibodies negatively affected only the number of LP sessions required to reach the collection goal, but no other PBSC mobilization/collection outcome parameters. In contrast, the probability of reaching a high collection goal of ≥6 × 10 CD34 cells/kg body weight was higher after lenalidomide-based induction compared to VCD/PAD or VAD - taking into account - that a higher G-SCF dosage was given in approximately one-third of patients receiving lenalidomide-based induction with/without antibodies.

CONCLUSION

Considering the identified risk factors in the clinical setting can contribute to optimized PBSC mobilization/collection. Moreover, our study demonstrates the necessity for a differentiated evaluation of PBSC mobilization/collection outcome parameters.

摘要

引言

大剂量化疗(HDCT)后进行自体血干细胞移植(ABSCT)仍然是新诊断的符合条件的多发性骨髓瘤(MM)患者的标准巩固治疗方法。作为前提条件,必须通过白细胞分离术(LP)动员并采集外周血干细胞(PBSC)。许多因素会妨碍PBSC的动员/采集。在此,我们对一大群患者的PBSC动员/采集结果参数进行了全面的多参数评估。

方法

总共纳入了790例在一线治疗期间接受PBSC动员/采集的MM患者(471例[60%]为男性,319例[40%]为女性)。评估的PBSC动员/采集结果参数包括PBSC动员的延长时间、普乐沙福的使用、LP疗程数以及PBSC总体采集目标/结果。

结果

741例(94%)患者接受了环磷酰胺/阿霉素/地塞米松(CAD)和粒细胞集落刺激因子(G-CSF)动员。80例(10%)患者使用了普乐沙福。489例(62%)患者及时开始了LP。530例(67%)患者在首次LP疗程时达到了PBSC采集目标。PBSC总体采集结果的平均值为10.3(标准差[SD]4.4)×10⁶个CD34⁺细胞/kg。在多参数分析中,与PBSC动员/采集结果呈负相关的变量为女性性别、年龄>60岁、国际分期系统(ISS)晚期以及诱导治疗前/期间的局部放疗,但不包括诱导治疗后的缓解状态。值得注意的是,所确定的风险因素对每个PBSC动员/采集结果参数的影响各不相同。在此背景下,与所有其他诱导方案相比,含/不含抗体的来那度胺诱导方案仅对达到采集目标所需的LP疗程数有负面影响,但对其他PBSC动员/采集结果参数没有影响。相比之下,与硼替佐米/阿霉素/地塞米松(VCD)/硼替佐米/阿霉素/地塞米松(PAD)或长春新碱/阿霉素/地塞米松(VAD)相比,含/不含抗体的来那度胺诱导方案后达到≥6×10⁶个CD34⁺细胞/kg体重的高采集目标的概率更高——考虑到在大约三分之一接受含/不含抗体的来那度胺诱导方案的患者中给予了更高剂量的G-SCF。

结论

在临床环境中考虑所确定的风险因素有助于优化PBSC的动员/采集。此外,我们的研究表明有必要对PBSC动员/采集结果参数进行差异化评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a9d/10601599/07c7ca5b4ca7/tmh-2023-0050-0005-530056_F01.jpg

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