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在blinatumomab 治疗复发/难治性急性淋巴细胞白血病期间,耐药和复发的相关性。

Correlates of resistance and relapse during blinatumomab therapy for relapsed/refractory acute lymphoblastic leukemia.

机构信息

Department of Hematology and Hematopoietic Cell Transplantation, Gehr Family Center for Leukemia Research, City of Hope Medical Center, Duarte, California.

Department of Information Sciences, Division of Biostatistics, City of Hope Medical Center, Duarte, California.

出版信息

Am J Hematol. 2017 Sep;92(9):858-865. doi: 10.1002/ajh.24783. Epub 2017 Jun 5.

Abstract

We retrospectively analyzed 65 patients with refractory/relapsed (r/r) ALL who were treated with blinatumomab for predictors of leukemia response as well as clinical patterns of relapse and resistance with particular focus on downregulation of CD19 expression and extramedullary disease (EM-ALL). The complete remission (CR) rate was 51%, and 15 (45%) responders underwent allogeneic hematopoietic cell transplantation (HCT) in CR. High leukemia burden (bone marrow blasts >50%) (P = .02), history of prior EM-ALL (P = .005), and active EM-ALL at the time of initiating blinatumomab (P = .05) predicted lower CR rate. Among refractory cases, 13 (41%) had evidence of EM-ALL progression, and CD19 expression was negative or dim in 18% and 23%, respectively. Among responders, 20 (61%) subsequently relapsed among whom EM-ALL relapse occurred in 8 (40%) patients, and CD19 expression was negative or dim in 35 and 6% of evaluable cases, respectively. Pretreatment moderate/strong CD19 expression (P = .01) and history of prior EM-ALL during ALL course (P = .04) were risk factors for developing EM-ALL at progression/relapse. However, no pretreatment factors predicted progression/relapse with CD19-negative ALL. Overall-survival (OS) and even-free survival were improved for patients underwent allogeneic HCT compared to responders who did not. Furthermore, OS was superior for patients responded to blinatumomab compared to those who did not. Extramedullary and CD19-negative disease are common during blinatumomab failure in r/r ALL. In addition to high leukemia burden, concurrent or prior history EM-ALL were associated with lower response to blinatumomab. Higher CD19 expression as well as prior history of EM-ALL were associated with EM-ALL at the time of blinatumomab failure.

摘要

我们回顾性分析了 65 例接受blinatumomab 治疗的难治/复发(r/r)ALL 患者,以预测白血病反应的预测因子,以及特别关注 CD19 表达下调和骨髓外疾病(EM-ALL)的复发和耐药的临床模式。完全缓解(CR)率为 51%,15 例(45%)应答者在 CR 时行异基因造血细胞移植(HCT)。高白血病负荷(骨髓原始细胞>50%)(P=0.02)、既往有 EM-ALL 病史(P=0.005)和blinatumomab 起始时存在活动性 EM-ALL(P=0.05)预测 CR 率较低。在难治性病例中,13 例(41%)有 EM-ALL 进展的证据,CD19 表达分别为阴性或弱表达,分别占 18%和 23%。在应答者中,20 例(61%)随后复发,其中 8 例(40%)发生 EM-ALL 复发,在可评估病例中,分别有 35%和 6%的病例 CD19 表达阴性或弱表达。预处理中度/强 CD19 表达(P=0.01)和 ALL 病程中既往有 EM-ALL 病史(P=0.04)是进展/复发时发生 EM-ALL 的危险因素。然而,没有预处理因素预测 CD19 阴性 ALL 的进展/复发。与未行异基因 HCT 的应答者相比,行异基因 HCT 的患者总生存(OS)和无事件生存均改善。此外,与未应答者相比,对 blinatumomab 有反应的患者的 OS 更好。在 r/r ALL 中,blinatumomab 失败时骨髓外和 CD19 阴性疾病很常见。除了白血病负荷高外,同时或既往有 EM-ALL 病史与对 blinatumomab 的反应较低相关。较高的 CD19 表达以及既往有 EM-ALL 病史与 blinatumomab 失败时发生 EM-ALL 相关。

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