ctDNA dynamics and mechanisms of acquired resistance in patients treated with osimertinib with or without bevacizumab from the randomised phase II ETOP-BOOSTER trial

IF 10 1区 医学 Q1 ONCOLOGY Clinical Cancer Research Pub Date : 2024-09-09 DOI:10.1158/1078-0432.ccr-24-0932
Ross A. Soo, Urania Dafni, Ji-Youn Han, Byoung Chul Cho, Ernest Nadal, Chong Ming Yeo, Enric Carcereny, Javier de Castro, Maria Angeles Sala, Linda Coate, Mariano Provencio, Christian Britschgi, Patrick Vagenknecht, Georgia Dimopoulou, Roswitha Kammler, Stephen P. Finn, Solange Peters, Rolf A. Stahel
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Abstract

Background: ETOP 10-16 BOOSTER study was a randomised phase II trial of osimertinib and bevacizumab versus osimertinib in patients with an acquired EGFR T790M mutation. The mechanisms of acquired resistance to osimertinib and bevacizumab have not been described previously. Methods: Next generation sequencing (Guardant360®) was conducted in serial plasma samples. The association between ctDNA and efficacy outcomes was explored and molecular alterations at progression were described. Results: 136 patients (88% of 155 randomised) had plasma samples at baseline (68 per arm), 110 (71%) at week 9 and 65 (42%) at progression. In a multivariable model for progression-free survival (PFS), the treatment effect was found different by smoking status (interaction p=0.046), with the effect of smoking also different by baseline EGFR T790M (interaction p=0.033), while both TP53 at baseline and tissue EGFR Exon 21 L858R mutation were significantly associated with worse PFS outcome. Smokers (current/former) without baseline EGFR T790M showed a significant improvement in PFS under combination treatment, albeit with small numbers (p=0.015). Week-9 EGFR T790M clearance was associated with improved PFS in the osimertinib arm (p=0.0097). Acquired EGFR C797S mutations were detected in 22% and 13% of patients in the combination and osimertinib arm, respectively. Conclusions: The differential effect of treatment by smoking was not explained by TP53 mutation or other molecular alterations examined. Molecular mechanisms of acquired resistance were detected but no novel molecular alterations were identified in the combination arm.
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随机II期ETOP-BOOSTER试验中接受奥希替尼联合或不联合贝伐珠单抗治疗的患者的ctDNA动态和获得性耐药机制
研究背景ETOP 10-16 BOOSTER研究是一项随机II期试验,在获得性表皮生长因子受体(EGFR)T790M突变患者中进行奥希替尼和贝伐单抗与奥希替尼的对比试验。奥希替尼和贝伐珠单抗的获得性耐药机制此前尚未描述。研究方法对连续血浆样本进行新一代测序(Guardant360®)。探讨了ctDNA与疗效之间的关联,并描述了进展期的分子改变。结果136名患者(占155名随机患者的88%)在基线时采集了血浆样本(每组68人),110人(71%)在第9周采集了血浆样本,65人(42%)在病情进展时采集了血浆样本。在无进展生存期(PFS)的多变量模型中,吸烟状态对治疗效果的影响不同(交互作用 p=0.046),基线 EGFR T790M 对吸烟的影响也不同(交互作用 p=0.033),而基线 TP53 和组织 EGFR 第 21 号外显子 L858R 突变与较差的 PFS 结果显著相关。没有基线表皮生长因子受体 T790M 的吸烟者(现吸烟者/曾经吸烟者)在接受联合治疗后 PFS 有明显改善,尽管人数不多(P=0.015)。在奥希替尼治疗组中,第9周EGFR T790M清除率与PFS改善相关(p=0.0097)。在联合用药和奥希替尼治疗组中,分别有22%和13%的患者检测到获得性表皮生长因子受体C797S突变。结论TP53突变或其他分子改变无法解释吸烟对治疗的不同影响。研究发现了获得性耐药的分子机制,但在联合治疗组中未发现新的分子改变。
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来源期刊
Clinical Cancer Research
Clinical Cancer Research 医学-肿瘤学
CiteScore
20.10
自引率
1.70%
发文量
1207
审稿时长
2.1 months
期刊介绍: Clinical Cancer Research is a journal focusing on groundbreaking research in cancer, specifically in the areas where the laboratory and the clinic intersect. Our primary interest lies in clinical trials that investigate novel treatments, accompanied by research on pharmacology, molecular alterations, and biomarkers that can predict response or resistance to these treatments. Furthermore, we prioritize laboratory and animal studies that explore new drugs and targeted agents with the potential to advance to clinical trials. We also encourage research on targetable mechanisms of cancer development, progression, and metastasis.
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