抗 CD38 单克隆抗体会损害多发性骨髓瘤患者的 CD34+ 动员能力并影响其克隆生成潜能。

IF 2.4 3区医学 Q2 HEMATOLOGY

Blood Transfusion Pub Date : 2024-07-01 DOI:10.2450/BloodTransfus.667

Arianna Zappaterra, Ivan Civettini, Anna Maria Cafro, Laura Pezzetti, Silvia Pierini, Michela Anghilieri, Laura Bellio, Paola Bertazzoni, Giovanni Grillo, Periana Minga, Maria L Pioltelli, Emanuele Ravano, Marianna Sassone, Clara V Viganò, Elisabetta B Volpato, Carlo Gambacorti-Passerini, Silvano Rossini, Roberto Cairoli, Roberto Crocchiolo

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引用次数: 0

摘要

背景：对于符合强化化疗条件的新诊断多发性骨髓瘤（NDMM）患者，目前的标准是先用达拉单抗诱导，然后进行自体干细胞移植。然而，人们担心达拉单抗治疗后对CD34+动员可能产生负面影响。在此，我们比较了达拉单抗和非达拉单抗疗法对NDMM患者的CD34+动员和克隆生成潜能的影响：分析了41例连续入组的NDMM患者的临床、动员和克隆生成数据。患者于2021年1月至2023年3月在意大利米兰的ASST Grande Ospedale Metropolitano Niguarda医院接受了自体CD34+采集。对BFU-E和CFU-GM进行了克隆生成性分析：75%的达拉土单抗治疗患者接受了1次以上的血液净化治疗，而非达拉土单抗治疗患者的这一比例为24%（P=0.0017）。达拉土单抗治疗患者的CD34+计数明显较低（平均值分别为38 vs 79/μL；p=0.0011），CD34+收获量中位数为3.98×106/kg（范围1.68-9.18），而非达拉土单抗治疗患者为6.87×106/kg（范围1.63-16.85）（p=0.0006）。在多变量分析中，年龄较大的患者（OR 1.2，95% CI 1-1.4，Z=2.10，p=0.03）和达拉曲单抗治疗的患者（OR 15，95% CI 2.8-129，p=0.004）接受>1次血液净化的可能性明显更高。此外，即使考虑到患者年龄和CD34+水平，基于达拉单抗的诱导治疗与BFU-E集落形成呈独立负相关（p=0.0148）：讨论：我们的研究结果强调了达拉单抗诱导治疗对NDMM患者CD34+动员的影响。接受达拉土单抗治疗的患者需要进行多次血液净化的概率更高。有趣的是，达拉土单抗可能会对BFU-E集落的形成产生负面影响，而与CD34+细胞数量无关，这一观察结果提供了新的生物学视角。血液净化团队应采取适当的策略来减轻这些潜在的负面影响。

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Anti-CD38 monoclonal antibody impairs CD34+ mobilization and affects clonogenic potential in multiple myeloma patients.

Background: Induction with daratumumab-based regimens followed by autologous stem cell transplantation is the current standard for newly diagnosed multiple myeloma (NDMM) patients eligible for intensive chemotherapy. However, concerns emerged regarding potential negative effects following daratumumab-based treatment on CD34+ mobilization. We here compared CD34+ mobilization and clonogenic potential between daratumumab and non-daratumumab based therapy without upfront plerixafor administration among patients affected by NDMM.

Materials and methods: Clinical, mobilization and clonogenic data from 41 consecutively enrolled NDMM patients were analyzed. Patients underwent collection of autologous CD34+ by apheresis at the ASST Grande Ospedale Metropolitano Niguarda, Milan, Italy, from January 2021 to March 2023. Clonogenicity analysis was performed on BFU-E and CFU-GM.

Results: Seventy-five percent of daratumumab-treated patients underwent >1 apheresis, compared to 24% of non-daratumumab patients (p=0.0017). Daratumumab-treated patients had significantly lower CD34+ count (mean 38 vs 79/μL, respectively; p=0.0011), with a median CD34+ harvest of 3.98×10⁶/kg (range 1.68-9.18) vs 6.87×10⁶/kg (range 1.63-16.85) in non-daratumumab-treated (p=0.0006). In multivariate analysis the likelihood of undergoing >1 apheresis was significantly higher in older patients (OR 1.2, 95% CI 1-1.4, Z=2.10, p=0.03) and daratumumab-treated patients (OR 15, 95% CI 2.8-129, p=0.004). Moreover, daratumumab-based induction therapy demonstrated an independent negative association with BFU-E colony formation (p=0.0148), even when accounting for patient age and CD34+ levels.

Discussion: Our findings underscore the impact of daratumumab-based treatment on CD34+ mobilization in a real-life, upfront plerixafor-free population of NDMM patients. Higher probability of requiring multiple apheresis occurred among daratumumab-treated patients. Interestingly, the observation that daratumumab might negatively impact BFU-E colony formation, independent of CD34+ cell count, offers novel biological perspectives. Appropriate strategies should be adopted by the Apheresis teams to mitigate these potential negative effects.

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来源期刊

Blood Transfusion HEMATOLOGY-

CiteScore

6.10

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2.70%

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2 months

期刊介绍： Blood Transfusion welcomes international submissions of Original Articles, Review Articles, Case Reports and Letters on all the fields related to Transfusion Medicine.