Marmouset Vincent, Decroocq Justine, Garciaz Sylvain, Etienne Gabriel, Belhabri Amine, Bertoli Sarah, Gastaud Lauris, Simand Célestine, Chantepie Sylvain, Uzunov Madalina, Genthon Alexis, Berthon Céline, Chiche Edmond, Dumas Pierre-Yves, Vargaftig Jacques, Salmeron Géraldine, Lemasle Emilie, Tavernier Emmanuelle, Delage Jérémy, Loirat Marion, Morineau Nadine, Blanc-Durand Félix, Pautier Patricia, Vergé Véronique, Auger Nathalie, Thomas Myrtille, Stefani Laetitia, Lepelley Marion, Boyer Thomas, Thepot Sylvain, Gourin Marie-Pierre, Bourquard Pascal, Duchmann Matthieu, Morice Pierre-Marie, Michallet Mauricette, Adès Lionel, Fenaux Pierre, Récher Christian, Dombret Hervé, Pagès Arnaud, Marzac Christophe, Leary Alexandra, Micol Jean-Baptiste
Department of Hematology, Gustave Roussy, Université Paris-Saclay, Villejuif, France.
Interception Program, Personalized Cancer Prevention Center, Gustave Roussy, Université Paris-Saclay, Villejuif, France.
Clin Cancer Res. 2022 Dec 1;28(23):5211-5220. doi: 10.1158/1078-0432.CCR-22-1622.
To provide insights into the diagnosis and management of therapy-related myeloid neoplasms (t-MN) following PARP inhibitors (PARPi).
In a French cancer center, we identified and described the profiles of 13 t-MN diagnosed among 37 patients with ovarian cancer referred to hematology consultation for cytopenia under PARPi. Next, we described these 13 t-MN post-PARPi among 37 t-MN post ovarian cancer according to PARPi exposure. Finally, we described 69 t-MN post-PARPi in a national cohort.
From 2016 to 2021, cumulative incidence of t-MN was 3.5% (13/373) among patients with ovarian cancer treated with PARPi. At time of hematologic consultation, patients with t-MN had a longer PARPi exposure (9 vs. 3 months, P = 0.01), lower platelet count (74 vs. 173 G/L, P = 0.0005), and more cytopenias (2 vs. 1, P = 0.0005). Compared with t-MN not exposed to PARPi, patients with t-MN-PARPi had more BRCA1/2 germline mutation (61.5% vs. 0%, P = 0.03) but similar overall survival (OS). In the national cohort, most t-MN post-PARPi had a complex karyotype (61%) associated with a high rate of TP53 mutation (71%). Median OS was 9.6 months (interquartile range, 4-14.6). In multivariate analysis, a longer time between end of PARPi and t-MN (HR, 1.046; P = 0.02), olaparib compared with other PARPi (HR, 5.82; P = 0.003) and acute myeloid leukemia (HR, 2.485; P = 0.01) were associated with shorter OS.
In a large series, we described a high incidence of t-MN post-PARPi associated with unfavorable cytogenetic and molecular abnormalities leading to poor OS. Early detection is crucial, particularly in cases of delayed cytopenia.
深入了解聚(ADP - 核糖)聚合酶抑制剂(PARPi)治疗后相关髓系肿瘤(t - MN)的诊断和管理。
在一家法国癌症中心,我们识别并描述了37例因PARPi治疗出现血细胞减少而转诊至血液科会诊的卵巢癌患者中确诊的13例t - MN的特征。接下来,我们根据PARPi暴露情况描述了这37例卵巢癌患者中13例PARPi治疗后的t - MN。最后,我们在一个全国队列中描述了69例PARPi治疗后的t - MN。
2016年至2021年,接受PARPi治疗的卵巢癌患者中t - MN的累积发病率为3.5%(13/373)。在血液科会诊时,t - MN患者的PARPi暴露时间更长(9个月对3个月,P = 0.01),血小板计数更低(74对173 G/L,P = 0.0005),血细胞减少更多(2种对1种,P = 0.0005)。与未暴露于PARPi的t - MN患者相比,PARPi治疗后的t - MN患者有更多的BRCA1/2种系突变(61.5%对0%,P = 0.03),但总生存期(OS)相似。在全国队列中,大多数PARPi治疗后的t - MN具有复杂核型(61%),与高比例的TP53突变(71%)相关。中位OS为9.6个月(四分位间距,4 - 14.6)。在多变量分析中,PARPi结束至t - MN的时间更长(风险比[HR],1.046;P = 0.02)、奥拉帕利与其他PARPi相比(HR,5.82;P = 0.003)以及急性髓系白血病(HR,2.485;P = 0.01)与较短的OS相关。
在一个大型系列研究中,我们描述了PARPi治疗后t - MN的高发病率,其与不良的细胞遗传学和分子异常相关,导致OS较差。早期检测至关重要,尤其是在出现延迟血细胞减少的情况下。
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