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Neurotoxicity and management of primary and secondary central nervous system lymphoma after adoptive immunotherapy with CD19-directed chimeric antigen receptor T-cells

医学 淋巴瘤 内科学 危险系数 免疫疗法 抗原 嵌合抗原受体 细胞因子释放综合征 原发性中枢神经系统淋巴瘤 免疫学 免疫系统 T细胞 置信区间
作者
Philipp Karschnia,Isabel Arrillaga‐Romany,April F. Eichler,Deborah Forst,Elizabeth R. Gerstner,Justin T. Jordan,Ina Ly,Scott R. Plotkin,Nancy Wang,Maria Martinez‐Lage,Sebastian Winter,Joerg‐Christian Tonn,Kai Rejeski,Louisa von Baumgarten,Daniel P. Cahill,Brian V. Nahed,Ganesh M. Shankar,Jeremy S. Abramson,Jeffrey A. Barnes,Areej El‐Jawahri,Ephraim P. Hochberg,P. Connor Johnson,Jacob D. Soumerai,Ronald W. Takvorian,Yi‐Bin Chen,Matthew J. Frigault,Jörg Dietrich
出处
期刊:Neuro-oncology [Oxford University Press]
卷期号:25 (12): 2239-2249 被引量:7
标识
DOI:10.1093/neuonc/noad118
摘要

Abstract Background Chimeric antigen receptor (CAR) T-cells targeting CD19 have been established as a leading engineered T-cell therapy for B-cell lymphomas; however, data for patients with central nervous system (CNS) involvement are limited. Methods We retrospectively report on CNS-specific toxicities, management, and CNS response of 45 consecutive CAR T-cell transfusions for patients with active CNS lymphoma at the Massachusetts General Hospital over a 5-year period. Results Our cohort includes 17 patients with primary CNS lymphoma (PCNSL; 1 patient with 2 CAR T-cell transfusions) and 27 patients with secondary CNS lymphoma (SCNSL). Mild ICANS (grade 1–2) was observed after 19/45 transfusions (42.2%) and severe immune effector cell-associated neurotoxicity syndrome (ICANS) (grade 3–4) after 7/45 transfusions (15.6%). A larger increase in C-reactive protein (CRP) levels and higher rates of ICANS were detected in SCNSL. Early fever and baseline C-reactive protein levels were associated with ICANS occurrence. CNS response was seen in 31 cases (68.9%), including a complete response of CNS disease in 18 cases (40.0%) which lasted for a median of 11.4 ± 4.5 months. Dexamethasone dose at time of lymphodepletion (but not at or after CAR T-cell transfusion) was associated with an increased risk for CNS progression (hazard ratios [HR] per mg/d: 1.16, P = .031). If bridging therapy was warranted, the use of ibrutinib translated into favorable CNS-progression-free survival (5 vs. 1 month, HR 0.28, CI 0.1–0.7; P = .010). Conclusions CAR T-cells exhibit promising antitumor effects and a favorable safety profile in CNS lymphoma. Further evaluation of the role of bridging regimens and corticosteroids is warranted.
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