Serial Circulating Tumor DNA Sequencing to Monitor Response and Define Acquired Resistance to Letrozole/Abemaciclib in Endometrial Cancer.

IF 5.6 2区医学 Q1 ONCOLOGY

JCO precision oncology Pub Date : 2025-04-01 Epub Date: 2025-04-10 DOI:10.1200/PO-24-00882

Panagiotis A Konstantinopoulos, Mingyang Cai, Elizabeth K Lee, Carolyn Krasner, Susana M Campos, Joyce F Liu, Neil S Horowitz, Meghan Shea, Heather A Parsons, Alexi A Wright, Sara Bouberhan, Richard T Penson, Oladapo Yeku, Martin Hayes, Hannah Sawyer, Madeline Polak, Cesar M Castro, Su-Chun Cheng, Caroline M Weipert, Ursula A Matulonis

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Abstract

Purpose: In a phase II study, letrozole/abemaciclib demonstrated an objective response rate of 30% and a median progression-free survival (PFS) of 9.1 months in recurrent estrogen receptor-positive endometrial cancer (EC). While tissue-based tumor profiling revealed several mechanistically relevant candidate baseline genomic predictors of response, circulating tumor DNA (ctDNA) is a less invasive alternative to monitor therapeutic efficacy and define acquired resistance.

Methods: Serial plasma specimens were obtained at baseline, C2D1, C3D1, C8D1, the time of objective response, and the time of progression. Samples were analyzed using the Guardant Reveal assay to assess methylation-based tumor fraction (TF), with the Guardant360 assay providing genotyping of >700 genes in samples with detectable ctDNA. Treatment response was assessed using a measure of the relative change in TF pre- versus on-treatment.

Results: A total of 99 of 102 (97%) samples from 28 patients were successfully analyzed. Patients with above median baseline TF exhibited worse median PFS (2.0 months v 16.5 months, P < .005, hazard ratio [HR], 24.1) and worse overall survival (OS) (10.7 months v not yet reached, P < .005, HR, 14.8). Patients with molecular response (MR) after the first or second cycle of letrozole/abemaciclib therapy had significantly better median PFS and OS regardless of the cutoff used for definition of MR. ctDNA analysis of postprogression specimens identified several acquired genomic alterations associated with resistance to letrozole/abemaciclib therapy in more than half of the patients, including PI3K pathway, receptor tyrosine kinase (FGFR1,2 and ERBB2 alterations), cell cycle pathway (RB1 and CCNE1 alterations), and ESR1 and MAPK pathway alterations. Two of the three patients with mismatch repair-deficient ECs acquired ESR1 mutations at the time of progression.

Conclusion: Baseline and on-treatment ctDNA dynamics may provide an early indication of benefit from letrozole/abemaciclib in EC. ctDNA at the time of progression may identify resistance alterations that may inform subsequent therapy.

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连续循环肿瘤DNA测序监测子宫内膜癌对来曲唑/阿贝马昔利的反应并确定获得性耐药。

目的：在一项II期研究中，来曲唑/abemaciclib治疗复发性雌激素受体阳性子宫内膜癌（EC）的客观缓解率为30%，中位无进展生存期（PFS）为9.1个月。虽然基于组织的肿瘤分析揭示了几种机制相关的候选基线基因组预测因子，但循环肿瘤DNA （ctDNA）是监测治疗效果和确定获得性耐药的一种侵入性较小的替代方法。方法：在基线、C2D1、C3D1、C8D1、客观反应时间和进展时间连续采集血浆标本。使用Guardant Reveal检测方法对样本进行分析，以评估基于甲基化的肿瘤分数（TF）， guarant360检测方法在可检测到ctDNA的样本中提供bb700个基因的基因分型。通过测量治疗前与治疗后TF的相对变化来评估治疗反应。结果：28例患者102份样本中，99份（97%）成功分析。高于中位基线TF的患者表现出更差的中位PFS（2.0个月vs 16.5个月，P < 0.005，危险比[HR]， 24.1）和更差的总生存期（OS）（10.7个月vs尚未达到，P < 0.005， HR, 14.8）。在来曲唑/abemaciclib治疗的第一个或第二个周期后出现分子反应（MR）的患者，无论用于MR定义的截止时间是多少，其中位PFS和OS都有明显更好的中位PFS和OS，对进展后标本的ctDNA分析发现，在一半以上的患者中，有几种获得性基因组改变与来曲唑/abemaciclib治疗的耐药性相关，包括PI3K途径、受体酪氨酸激酶（FGFR1、2和ERBB2改变）。细胞周期通路（RB1和CCNE1通路改变），以及ESR1和MAPK通路改变。三名错配修复缺陷的ECs患者中有两名在进展时获得了ESR1突变。结论：基线和治疗时的ctDNA动态可能提供来曲唑/阿贝马昔利治疗EC的早期适应症。进展时的ctDNA可以识别耐药性变化，从而为后续治疗提供信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

JCO precision oncology ONCOLOGY-

CiteScore

9.10

自引率

4.30%

发文量

363