Early Circulating Tumor DNA Shedding Kinetics for Prediction of Platinum Sensitivity in Patients With Small Cell Lung Cancer.

IF 5.3 2区医学 Q1 ONCOLOGY JCO precision oncology Pub Date : 2024-09-01 DOI:10.1200/PO.24.00216

Yonina R Murciano-Goroff, Angela B-Y Hui, Jose A Araujo Filho, Emily G Hamilton, Jacob J Chabon, Everett J Moding, Rene F Bonilla, Emily S Lebow, Daniel Gomez, Andreas Rimner, Michelle S Ginsberg, Michael Offin, Ritika Kundra, Viola Allaj, Larry Norton, Jorge S Reis-Filho, Pedram Razavi, Alexander Drilon, David R Jones, James M Isbell, W Victoria Lai, Charles M Rudin, Ash A Alizadeh, Bob T Li, Maximilian Diehn

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Abstract

Purpose: Small cell lung cancer (SCLC) is characterized by rapid progression after platinum resistance. Circulating tumor (ctDNA) dynamics early in treatment may help determine platinum sensitivity.

Materials and methods: Serial plasma samples were collected from patients receiving platinum-based chemotherapy for SCLC on the first 3 days of cycle one and on the first days of subsequent cycles with paired samples collected both before and again after infusions. Tumor-informed plasma analysis was carried out using CAncer Personalized Profiling by deep Sequencing (CAPP-Seq). The mean variant allele frequency (VAF) of all pretreatment mutations was tracked in subsequent blood draws and correlated with radiologic response.

Results: ctDNA kinetics were assessed in 122 samples from 21 patients. Pretreatment VAF did not differ significantly between patients who did and did not respond to chemotherapy (mean 22.5% v 4.6%, P = .17). A slight increase in ctDNA on cycle 1, day 1 immediately post-treatment was seen in six of the seven patients with available draws (fold change from baseline: 1.01-1.44), half of whom achieved a response. All patients who responded had a >2-fold decrease in mean VAF on cycle 2 day 1 (C2D1). Progression-free survival (PFS) and overall survival (OS) were significantly longer in patients with a >2-fold decrease in mean VAF after one treatment cycle (6.8 v 2.6 months, log-rank P = .0004 and 21.7 v 6.4 months, log rank P = .04, respectively).

Conclusion: A >2-fold decrease in ctDNA concentration was observed by C2D1 in all patients who were sensitive to platinum-based therapy and was associated with longer PFS and OS.

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用于预测小细胞肺癌患者铂敏感性的早期循环肿瘤 DNA 脱落动力学

目的：小细胞肺癌（SCLC）的特点是铂类耐药后进展迅速。治疗早期的循环肿瘤（ctDNA）动态有助于确定铂类药物的敏感性：在接受以铂类为基础的化疗的 SCLC 患者中，在第一周期的前 3 天和后续周期的第一天收集连续血浆样本，并在输液前和输液后再次收集配对样本。利用深度测序肿瘤个体化分析（CAPP-Seq）对血浆进行了肿瘤信息分析。在随后的抽血中跟踪所有治疗前突变的平均变异等位基因频率（VAF），并将其与放射学反应相关联。治疗前 VAF 在对化疗有反应和无反应的患者之间无明显差异（平均 22.5% 对 4.6%，P = .17）。在有抽样结果的七名患者中，有六名患者的ctDNA在治疗后第1周期第1天出现轻微增加（与基线相比的折叠变化：1.01-1.44），其中半数患者出现了反应。所有有应答的患者在第 2 周期第 1 天（C2D1）的平均 VAF 均下降了 2 倍以上。一个治疗周期后平均VAF下降>2倍的患者的无进展生存期（PFS）和总生存期（OS）明显更长（分别为6.8个月对2.6个月，对数秩P = .0004和21.7个月对6.4个月，对数秩P = .04）：结论：在所有对铂类疗法敏感的患者中，C2D1可观察到ctDNA浓度下降2倍以上，并与更长的PFS和OS相关。

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