Waldenström巨球蛋白血症患者是否应该接受BTK抑制剂作为一线治疗?

IF 0.9 Q4 HEMATOLOGY
Hemato Pub Date : 2022-10-23 DOI:10.3390/hemato3040046
M. Deodato, A. Frustaci, G. Zamprogna, G. Cotilli, R. Cairoli, A. Tedeschi
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引用次数: 0

摘要

Waldenström巨球蛋白血症(WM)是一种罕见的惰性淋巴瘤,具有异质性临床表现。由于没有随机试验表明治疗初期患者的最佳治疗方案,指南建议利妥昔单抗联合方案或BTK抑制剂(BTKi)作为可行的替代方案。决策过程中有几个因素:患者的年龄和体质、疾病特征和基因型。化学免疫疗法(CIT)是一种持续时间固定、成本较低且有效的选择,即使在基因型不利的患者中也能延长下一次治疗的时间。免疫抑制和与治疗相关的第二种癌症可能是严重的问题。基于蛋白酶体抑制剂的方案在快速控制疾病方面是有效的,尽管硼替佐米相关的神经病变阻碍了这些药物的选择,并且老年人的治疗方案可能不容易控制。BTKi表现出高反应率和延长生存期,以及口服给药的便利性和有限的细胞减少。然而,结果受到基因型的影响,一些问题仍然存在,特别是持续的药物暴露可能导致额外的血液并发症和耐药性。尽管下一代BTKi提高了治疗耐受性,但是否应该将BTKi作为一线治疗提供给每位患者的问题仍存在争议。CIT具有固定的持续时间安排、延长的下一次治疗时间和独立于基因型的结果,仍然是我们在WM中的首选。然而,对于不适合CIT的虚弱患者,BTKi仍然是一个有价值的选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Should Patients with Waldenström Macroglobulinemia Receive a BTK Inhibitor as Frontline Therapy?
Waldenström Macroglobulinemia (WM) is a rare indolent lymphoma with heterogeneous clinical presentation. As there are no randomised trials suggesting the best treatment option in treatment-naive patients, guidelines suggest either rituximab-combining regimens or BTK-inhibitors (BTKi) as feasible alternatives. Several factors play in the decision-making process: patients’ age and fitness, disease characteristics and genotype. Chemoimmunotherapy (CIT) represents a fixed-duration, less expensive and effective option, able to achieve prolonged time-to-next treatment even in patients with unfavourable genotypes. Immunosuppression and treatment-related second cancers may represent serious concerns. Proteasome-inhibitor-based regimens are effective with rapid disease control, although bortezomib-related neuropathy discourages the choice of these agents and treatment schedules may not be easily manageable in the elderly. BTKi have demonstrated high rates of response and prolonged survival together with the convenience of an oral administration and limited cytopenias. However, outcomes are impacted by genotype and some concerns remain, in particular the continuous drug exposure that may result in extra-haematological complications and drug resistance. Although next-generation BTKi have improved treatment tolerance, the question whether BTKi should be offered as frontline therapy to every patient is still debated. Giving fixed-duration schedule, prolonged time-to-next treatment and outcomes independent of genotype, CIT is still our preferred choice in WM. However, BTKi remain a valuable option in frail patients unsuitable for CIT.
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来源期刊
CiteScore
1.30
自引率
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