54例不适合大剂量化疗的原发性中枢神经系统淋巴瘤患者首次脑复发或进展后的生存、预后因素、住院时间和临床表现状况:回顾性分析

Neurological Research and Practice Pub Date : 2023-02-23 DOI:10.1186/s42466-023-00234-y

Sabine Seidel, Thomas Kowalski, Verena Nilius-Eliliwi, Roland Schroers, Uwe Schlegel

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引用次数: 2

摘要

背景:复发或难治性原发性中枢神经系统淋巴瘤(r/r PCNSL)的治疗是困难的，特别是那些不适合自体干细胞移植(hdl - asct)进行大剂量化疗的患者。目前还没有针对这些患者的标准治疗方法。方法:我们回顾性分析54例不符合hcc - asct条件的单纯脑复发或进展的r/r PCNSL患者(n = 23难治性，n = 31复发)治疗前后的生存率、预后因素、住院时间和Karnofsky性能评分(KPS)。结果:治疗方案为替莫唑胺(+利妥昔单抗)(n = 21)、以高剂量甲氨蝶呤(HD-MTX)为基础的治疗(n = 11)、全脑放疗(WBRT)/局灶放疗(n = 11)、其他全身治疗(n = 2)和最佳支持治疗(BSC, n = 9)。中位无进展生存期(PFS)和总生存期(OS)分别为2.6个月(95% CI 1.0-4.2个月)和4.8个月(95% CI 3.3-6.3个月)。8例患者存活时间≥3年(13.1%，n = 3例接受替莫唑胺治疗，n = 3例接受WBRT治疗，n = 2例接受hd - mtx治疗)。应用任何挽救性治疗(vs. BSC)、复发年龄更小和无症状复发(vs.有症状)是积极的预后因素。不同抢救方法的OS无显著差异。替莫唑胺(+利妥昔单抗)/放疗治疗的中位住院时间为15/13天，而基于hd - mtx治疗的中位住院时间为55天。可评估患者(n = 41)的中位KPS在治疗前为60(范围30-100)，治疗后为50(范围20-90)。在对治疗有反应的患者(n = 16)中，KPS从治疗前的60(范围40-90)改善到治疗后的70(范围50-90)，而PD患者(n = 25)从60(范围30-100)恶化到40(范围20-70)。结论:孤立性脑复发或进展的r/r PCNSL患者的生存率较差。考虑到长期住院与基于hd - mtx的化疗相关以及与WBRT相关的神经毒性，替莫唑胺可能值得考虑，有机会延长生存期并避免长期住院。迫切需要新的治疗药物来提高r/r PCNSL患者的生存率。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Survival, prognostic factors, hospitalization time and clinical performance status after first cerebral relapse or progression in 54 patients with primary CNS lymphoma not eligible for high dose chemotherapy: a retrospective analysis.

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Background: Treatment of relapsed or refractory primary CNS lymphoma (r/r PCNSL) is difficult, particularly in patients not eligible for high dose chemotherapy with autologous stem cell transplantation (HDC-ASCT). No standard treatment has been defined for these patients yet.

Methods: We retrospectively analyzed survival, prognostic factors, hospitalization time and Karnofsky performance score (KPS) before and after treatment in 54 r/r PCNSL patients with isolated cerebral relapse or progression (n = 23 refractory, n = 31 relapsed) not eligible for HDC-ASCT, who received heterogenous salvage treatments.

Results: Treatments were temozolomide (+ rituximab) (n = 21), high dose methotrexate (HD-MTX)-based therapy (n = 11), whole brain radiotherapy (WBRT)/focal radiotherapy (n = 11), other systemic treatments (n = 2) and best supportive care (BSC, n = 9). Median progression free survival (PFS) and overall survival (OS) were 2.6 months (95% CI 1.0-4.2 months) and 4.8 months (95% CI 3.3-6.3 months), respectively. Eight patients survived for ≥ 3 years (13.1%, n = 3 received temozolomide, n = 3 WBRT, n = 2 HD-MTX-based treatment). Application of any salvage treatment (vs. BSC), younger age at relapse and asymptomatic (vs. symptomatic) relapse were positive prognostic factors. No significant differences in OS were found for the different salvage treatments. Median hospitalization time for treatment was 15/13 days for temozolomide (+ rituximab)/radiotherapy compared to 55 days for HD-MTX-based therapy. Median KPS in assessable patients (n = 41) was 60 (range 30-100) before treatment and 50 (range 20-90) after treatment. In patients with response to treatment (n = 16) KPS improved from 60 (range 40-90) before treatment to 70 (range 50-90) after treatment, while patients with PD (n = 25) deteriorated from 60 (range 30-100) to 40 (range 20-70).

Conclusion: Survival for this cohort of r/r PCNSL patients with isolated cerebral relapse or progression was poor. Considering long hospital stays associated with HD-MTX-based chemotherapy and neurotoxicity associated with WBRT, temozolomide might be worth considering with a chance of prolonged survival and avoidance of long hospitalization. Novel therapeutic agents are urgently needed to improve survival in r/r PCNSL patients.

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Neurological Research and Practice

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