Wozniak Agnieszka, Boeckx Bram, Modave Elodie, Weaver Amy, Lambrechts Diether, Littlefield Bruce A, Schöffski Patrick
Laboratory of Experimental Oncology, Department of Oncology, KU Leuven, Leuven, Belgium.
Laboratory of Translational Genetics, KU Leuven and VIB Center for Cancer Biology, Leuven, Belgium.
Clin Cancer Res. 2021 Jun 1;27(11):3106-3115. doi: 10.1158/1078-0432.CCR-20-4315. Epub 2021 Apr 1.
A randomized phase III study evaluated the efficacy of eribulin versus dacarbazine in patients with advanced liposarcoma and leiomyosarcoma. Improved overall survival (OS) led to approval of eribulin for liposarcoma, but not for leiomyosarcoma.
We explored the molecular profile of 77 archival leiomyosarcoma samples from this trial to identify potential predictive biomarkers, utilizing low-coverage whole-genome and whole-exome sequencing. Tumor molecular profiles were correlated with clinical data, and disease control was defined as complete/partial response or stable disease (RECIST v1.1).
Overall, 111 focal copy-number alterations were observed in leiomyosarcoma. Gain of chromosome 17q12 was the most common event, present in 43 of 77 cases (56%). In the eribulin-treated group, gains of 4q26, 20p12.2, 13q13.3, 8q22.2, and 8q13.2 and loss of 1q44 had a negative impact on progression-free survival (PFS), while loss of 2p12 correlated with better prognosis. Gains of 4q22.1 and losses of 3q14.2, 2q14.1, and 11q25 had a negative impact on OS in patients with leiomyosarcoma receiving eribulin. The most commonly mutated genes were (38%), (32%), and (17%). The presence of mutations had a negative impact on PFS in both treatment arms; however, the correlation with worse OS was observed only in the eribulin-treated patients. mutations were associated with longer PFS on eribulin.
Leiomyosarcoma has a complex genetic background, with multiple copy-number alterations and mutations affecting genes implicated in tumorigenesis. We identified several molecular changes with potential impact on survival of patients with leiomyosarcoma when treated with eribulin.
一项随机III期研究评估了艾日布林与达卡巴嗪在晚期脂肪肉瘤和平滑肌肉瘤患者中的疗效。总体生存期(OS)的改善使得艾日布林被批准用于脂肪肉瘤,但未被批准用于平滑肌肉瘤。
我们利用低覆盖度全基因组和全外显子测序,对该试验中的77份存档平滑肌肉瘤样本的分子特征进行了探索,以识别潜在的预测生物标志物。肿瘤分子特征与临床数据相关联,疾病控制被定义为完全缓解/部分缓解或疾病稳定(RECIST v1.1)。
总体而言,在平滑肌肉瘤中观察到111个局灶性拷贝数改变。17q12染色体增益是最常见的事件,77例中有43例(56%)出现该情况。在接受艾日布林治疗的组中,4q26、20p12.2、13q13.3、8q22.2和8q13.2的增益以及lq44的缺失对无进展生存期(PFS)有负面影响,而2p12的缺失与较好的预后相关。在接受艾日布林治疗的平滑肌肉瘤患者中,4q22.1的增益以及3q14.2、2q14.1和11q25的缺失对OS有负面影响。最常发生突变的基因是(38%)、(32%)和(17%)。在两个治疗组中,的存在对PFS均有负面影响;然而,仅在接受艾日布林治疗的患者中观察到与较差OS的相关性。突变与接受艾日布林治疗时更长的PFS相关。
平滑肌肉瘤具有复杂的遗传背景,存在多个影响肿瘤发生相关基因的拷贝数改变和突变。我们识别出了几种分子变化,这些变化在平滑肌肉瘤患者接受艾日布林治疗时可能对其生存产生影响。
