卵巢癌和多(ADP-核糖)聚合酶抑制剂后骨髓性肿瘤患者的基因型 BRCA 致病变体

IF 7.1 2区 医学 Q1 ONCOLOGY
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引用次数: 0

摘要

背景在接受多聚(ADP-核糖)聚合酶(PARP)抑制剂(PARPis)治疗的晚期高级别卵巢癌(aHGOC)患者中、生殖系 BRCA 致病变体(gBRCA-PV)的存在可能会增加骨髓诱变的风险,导致细胞毒治疗后骨髓增生异常性肿瘤(MDS-pCT)或急性髓性白血病(AML-pCT),因为它在造血祖细胞中也有杂合表达。我们的目的是根据 gBRCA-PV 状态调查 PARPi 后 MDSs/AMLs-pCT 的发生情况。患者和方法我们开展了一项回顾性单中心研究,以评估 2017 年 2 月至 2022 年 12 月期间接受至少 8 周维持性 PARPi 治疗且已知 gBRCA-PV 状态的 aHGOC 患者的 MDS/AML-pCT。终点是gBRCA-PV携带者和非携带者在接受PARPi治疗期间和治疗后发生MDSs-pCT和AMLs-pCT的患者比例:95人(57%)为gBRCA-PV携带者,72%的患者因疾病复发接受了PARPi治疗。gBRCA-PV携带者和非携带者接受PARPi治疗前后的化疗次数、中位总生存期和中位随访时间相当。在中位随访 40.0 个月(95% 置信区间:35.7-44.3)后,10 例(6%)患者被诊断为 MDS-pCT,4 例(2%)患者被诊断为 AML-pCT。在 gBRCA-PV 携带者中观察到 MDSs/AMLs-pCT 的比例较高(10% 对 2%;P = 0.16),尤其是 MDSs-pCT 的比例较高(9% 对 1%;P = 0.04)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Germline BRCA pathogenic variants in patients with ovarian cancer and post-poly (ADP-ribose) polymerase inhibitor myeloid neoplasms

Background

Among patients with advanced high-grade ovarian carcinoma (aHGOC) treated with poly (ADP-ribose) polymerase (PARP) inhibitors (PARPis), the presence of a germline BRCA pathogenic variant (gBRCA-PV) may increase the risk of bone marrow mutagenesis resulting in postcytotoxic therapy myelodysplastic neoplasms (MDS-pCT) or acute myeloid leukemia (AML-pCT), as it is expressed in heterozygosity also by hematopoietic progenitors. We aimed to investigate the occurrence of post-PARPi MDSs/AMLs-pCTs according to gBRCA-PV status.

Patients and methods

We conducted a retrospective single-center study to evaluate MDS/AML-pCT in patients with aHGOC and a known gBRCA-PV status receiving at least 8 weeks of maintenance PARPi, in any line of therapy, from February 2017 to December 2022. The endpoint was the proportion of patients who experienced MDSs-pCT and AMLs-pCT during and after treatment with PARPi, in gBRCA-PV carriers and non-carriers.

Results

A total of 166 patients were included: 95 (57%) had a gBRCA-PV and 72% received PARPi for recurrent disease. The number of lines of chemotherapies before and after PARPi, median overall survival, and median follow-up were comparable between gBRCA-PV carriers and non-carriers. After a median follow-up of 40.0 (95% confidence interval: 35.7-44.3) months, 10 (6%) patients were diagnosed with an MDS-pCT and 4 (2%) with an AML-pCT. A higher proportion of MDSs/AMLs-pCT (10% versus 2%; P = 0.16) and, in particular, of MDSs-pCT (9% versus 1%; P = 0.04) was observed among gBRCA-PV carriers.

Conclusions

The presence of a gBRCA-PV is associated with a higher risk of MDS-pCT and possibly of myeloid neoplasms after PARPi in patients with aHGOC who received PARPi, especially in the setting of recurrent disease.

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来源期刊
ESMO Open
ESMO Open Medicine-Oncology
CiteScore
11.70
自引率
2.70%
发文量
255
审稿时长
10 weeks
期刊介绍: ESMO Open is the online-only, open access journal of the European Society for Medical Oncology (ESMO). It is a peer-reviewed publication dedicated to sharing high-quality medical research and educational materials from various fields of oncology. The journal specifically focuses on showcasing innovative clinical and translational cancer research. ESMO Open aims to publish a wide range of research articles covering all aspects of oncology, including experimental studies, translational research, diagnostic advancements, and therapeutic approaches. The content of the journal includes original research articles, insightful reviews, thought-provoking editorials, and correspondence. Moreover, the journal warmly welcomes the submission of phase I trials and meta-analyses. It also showcases reviews from significant ESMO conferences and meetings, as well as publishes important position statements on behalf of ESMO. Overall, ESMO Open offers a platform for scientists, clinicians, and researchers in the field of oncology to share their valuable insights and contribute to advancing the understanding and treatment of cancer. The journal serves as a source of up-to-date information and fosters collaboration within the oncology community.
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