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[布雷西尤单抗自体白细胞介素治疗高危套细胞淋巴瘤的疗效与毒性:一例临床病例描述]

[Efficacy and toxicity of brexucabtagene autoleucel in the treatment of high-risk mantle cell lymphoma: description of a clinical case].

作者信息

Novo Mattia, Savelli Corrado Benevolo, Botto Barbara, Freilone Roberto

机构信息

SC Ematologia, Aou Città della Salute e della Scienza di Torino.

出版信息

Recenti Prog Med. 2025 Mar;116(3):e45-e49. doi: 10.1701/4460.44569.

DOI:10.1701/4460.44569
PMID:40084459
Abstract

INTRODUCTION

Relapsed or refractory (R/R) mantle cell lymphoma (MCL) represent a setting at unfavourable prognosis. Chimeric antigen receptor T-cells (CAR-T) are recently introduced in clinical practice as a new therapeutic option for this setting.

CLINICAL CASE

61-year-old man with MCL pleomorphic variant, TP53 mutated with high risk MIPI-c early relapsed after frontline immunochemotherapy and ibrutinib. It has treated with brexucabtagene autoleucel (brexu-cel) as third line. A complete remission (CR) is obtained at 1 moth post infusion but the patient developed a severe and prolonged hematological toxicity: anemia G4, thrombocytopenia G4, neutropenia G4. Three months post-CAR-T infusion eltrombopag is introduced with rapid hemoglobin and platelet count recovery and an improvement in neutrophil count but persistent G3 neutropenia at 2 years of follow up. The bone marrow biopsy revealed a granulocytic hypoplasia with a clonal hemopoiesis (ASLX1 and DNMT3A mutations encountered) at the next generation sequencing test (NGS). The patient is in persistent CR at 2 years post brexu-cel infusion without major infection encountered.

CONCLUSIONS

Brexu-cel represents an effective treatment option even in R/R MCL with high-risk features but can be associated with prolonged toxicities. An accurate patient selection and a close monitoring during post-CAR-T follow-up is crucial in order to prolong survival of these patients.

摘要

引言

复发或难治性(R/R)套细胞淋巴瘤(MCL)预后不佳。嵌合抗原受体T细胞(CAR-T)最近作为这种情况下的一种新治疗选择引入临床实践。

临床病例

一名61岁男性,患有MCL多形性变体,TP53突变,高风险MIPI-c,一线免疫化疗和伊布替尼治疗后早期复发。接受了布雷西尤单抗(brexu-cel)作为三线治疗。输注后1个月获得完全缓解(CR),但患者出现了严重且持续时间长的血液学毒性:4级贫血、4级血小板减少、4级中性粒细胞减少。CAR-T输注后3个月引入艾曲泊帕,血红蛋白和血小板计数迅速恢复,中性粒细胞计数有所改善,但随访2年时仍持续存在3级中性粒细胞减少。骨髓活检显示粒细胞发育不全,下一代测序检测(NGS)发现克隆性造血(发现ASLX1和DNMT3A突变)。布雷西尤单抗输注后2年,患者持续处于CR状态,未发生重大感染。

结论

布雷西尤单抗即使在具有高风险特征的R/R MCL中也是一种有效的治疗选择,但可能与延长的毒性相关。准确的患者选择和CAR-T治疗后随访期间的密切监测对于延长这些患者的生存期至关重要。

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