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Primary breast diffuse large B‐cell lymphoma in the rituximab era: Therapeutic strategies and patterns of failure

机译:利妥昔单抗时代的原发性乳腺弥漫性大B细胞淋巴瘤:治疗策略和失败模式

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摘要

Primary breast diffuse large B‐cell lymphoma (PB‐DLBCL) is a rare subtype of DLBCL with limited data on patterns of failure. This multicenter study aimed to define the optimum treatment strategy and patterns of failure for PB‐DLBCL patients. We retrospectively reviewed data on 108 PB‐DLBCL patients from 21 Chinese medical centers. Only patients with localized disease (involvement of breast and localized lymph nodes) were included. After a median follow‐up of 3.2 years, 32% of patients developed progression or relapse. A continuous pattern of relapse was observed, characterized by frequent late relapses in the contralateral breast and central nervous system (CNS). Although rituximab significantly reduced the overall cumulative risk of progression or relapse (5‐year cumulative risk 57% vs 24%, P = .029), it had limited effect on the reduction of breast relapse (P = .46). Consolidative radiotherapy significantly decreased the risk of breast relapse, even in the subgroup of patients treated with rituximab (5‐year cumulative risk 21.2% vs 0%, P = .012). A continuous risk of CNS progression or relapse up to 8.2 years from diagnosis was observed (10‐year cumulative risk 28.3%), with a median time to CNS relapse of 3.1 years. Neither rituximab nor prophylactic intrathecal chemotherapy significantly decreased the risk of CNS relapse. In summary, our study indicates that PB‐DLBCL has a continuous pattern of relapse, especially with frequent late relapses in the CNS and contralateral breast. Rituximab and RT confer complementary benefit in the reduction of relapse. However, neither the addition of rituximab nor prophylactic intrathecal chemotherapy could effectively prevent CNS relapse for style="fixed-case">PB‐ style="fixed-case">DLBCL patients.
机译:原发性乳腺弥漫性大B细胞淋巴瘤(PB‐DLBCL)是DLBCL的罕见亚型,其失败模式的数据有限。这项多中心研究旨在确定PB‐DLBCL患者的最佳治疗策略和失败模式。我们回顾性审查了来自21个中国医学中心的108名PB-DLBCL患者的数据。仅包括局部疾病(累及乳房和局部淋巴结)的患者。中位随访3.2年后,32%的患者出现了进展或复发。观察到连续的复发模式,其特征在于对侧乳房和中枢神经系统(CNS)频繁晚期复发。尽管利妥昔单抗显着降低了进展或复发的总体累积风险(5年累积风险为57%vs 24%,P = .029),但对降低乳腺癌复发的作用有限(P = .46)。即使在接受利妥昔单抗治疗的患者亚组中,合并放疗也显着降低了乳腺癌复发的风险(5年累积风险为21.2%vs 0%,P = .012)。从诊断到发现CNS持续或复发的持续风险长达8.2年(10年累积风险为28.3%),中枢神经系统复发的中位时间为3.1年。利妥昔单抗和预防性鞘内化疗均未显着降低中枢神经系统复发的风险。总而言之,我们的研究表明PB‐DLBCL具有连续的复发模式,尤其是中枢神经系统和对侧乳腺的频繁晚期复发。利妥昔单抗和RT在减少复发方面具有互补的优势。然而,对于 style =“ fixed-case”> PB - style =“ fixed-case”> DLBCL 患者,添加利妥昔单抗或预防性鞘内化疗均不能有效预防CNS复发。

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