简要报告:表皮生长因子受体突变型 NSCLC 小细胞转化的综合临床基因组学分析为潜在治疗靶点提供信息

Bingnan Zhang MD, MBA , Whitney Lewis PharmD , C. Allison Stewart PhD , Benjamin B. Morris PhD , Luisa M. Solis MD , Alejandra Serrano MD , Yuanxin Xi PhD , Qi Wang PhD , Elyse R. Lopez MD , Kyle Concannon MD , Simon Heeke PhD , Ximing Tang MD, PhD , Gabriela Raso MD , Robert J. Cardnell PhD , Natalie Vokes MD , George Blumenschein MD , Yasir Elamin MD , Frank Fosella MD , Anne Tsao MD , Ferdinandos Skoulidis MD, PhD , Xiuning Le MD, PhD
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Previous reports revealed transformed SCLC from <em>EGFR</em>-mutant NSCLC portends very poor prognosis and lack effective treatment. Genomic analyses revealed <em>TP53</em> and <em>RB1</em> loss of function increase the risk of SCLC transformation. Little has been reported on the detailed clinicogenomic characteristics and potential therapeutic targets for this patient population.</p></div><div><h3>Methods</h3><p>In this study, we conducted a single-center retrospective analysis of clinical and genomic characteristics of patients with <em>EGFR</em>-mutant NSCLC transformed to SCLC. Demographic data, treatment course, and clinical molecular testing reports were extracted from electronic medical records. Kaplan-Meier analyses were used to estimate survival outcomes. Next generation sequencing-based assays was used to identify <em>EGFR</em> and co-occurring genetic alterations in tissue or plasma before and after SCLC transformation. 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引用次数: 0

摘要

导言NSCLC向SCLC转化的最佳特征是表皮生长因子受体(EGFR)突变的NSCLC,而新出现的病例报告也出现在ALK、RET和KRAS变异的NSCLC中。以往的报告显示,由表皮生长因子受体突变 NSCLC 转化而来的 SCLC 预后极差,且缺乏有效的治疗方法。基因组分析显示,TP53 和 RB1 功能缺失会增加 SCLC 转化的风险。本研究对EGFR突变NSCLC转化为SCLC患者的临床和基因组特征进行了单中心回顾性分析。我们从电子病历中提取了人口统计学数据、治疗过程和临床分子检测报告。采用卡普兰-梅耶尔分析估计生存结果。采用基于新一代测序技术的检测方法来鉴定SCLC转化前后组织或血浆中的表皮生长因子受体(EGFR)和并发基因改变。对一名EGFR-NSCLC转化的SCLC肿瘤患者产生的患者衍生异种移植模型进行了单细胞RNA测序(scRNA-seq)。初诊时的中位年龄为 58 岁,发生 SCLC 转化的中位时间为 24.2 个月。68%的患者为女性,82%的患者从不吸烟。79%的患者被诊断为IV期疾病,超过一半的患者在基线时有脑转移。整个组群的中位总生存期为自初次诊断起38.3个月,自SCLC转化起12.4个月。大多数患者存在表皮生长因子受体19外显子缺失,而非21外显子L858R改变。与我们队列中停止使用酪氨酸激酶抑制剂的患者相比,转化后继续使用表皮生长因子受体酪氨酸激酶抑制剂并不能改善总生存率。在20个配对的转化前和转化后患者样本中,转化后的PIK3CA改变在统计学上有显著的富集(p = 0.04)。纵向液体活检样本的图谱分析表明,TP53、RB1和PIK3CA基因改变的变异等位基因频率不断增加,表明在活检证实SCLC之前就出现了SCLC基因改变。ScRNA-seq揭示了潜在的治疗靶点,包括DLL3、CD276 (B7-H3)和PTK7在转化的SCLC中广泛表达。在我们的 34 例表皮生长因子受体突变 NSCLC 队列中,观察到 SCLC 转化后预后较差。对配对样本和纵向样本进行的临床基因组学分析确定了转化后出现的基因组改变,scRNA-seq揭示了这一人群中的潜在治疗靶点。还需要进一步的研究来严格验证这一患者群体的生物标志物和治疗靶点。
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Brief Report: Comprehensive Clinicogenomic Profiling of Small Cell Transformation From EGFR-Mutant NSCLC Informs Potential Therapeutic Targets

Introduction

NSCLC transformation to SCLC has been best characterized with EGFR-mutant NSCLC, with emerging case reports seen in ALK, RET, and KRAS-altered NSCLC. Previous reports revealed transformed SCLC from EGFR-mutant NSCLC portends very poor prognosis and lack effective treatment. Genomic analyses revealed TP53 and RB1 loss of function increase the risk of SCLC transformation. Little has been reported on the detailed clinicogenomic characteristics and potential therapeutic targets for this patient population.

Methods

In this study, we conducted a single-center retrospective analysis of clinical and genomic characteristics of patients with EGFR-mutant NSCLC transformed to SCLC. Demographic data, treatment course, and clinical molecular testing reports were extracted from electronic medical records. Kaplan-Meier analyses were used to estimate survival outcomes. Next generation sequencing-based assays was used to identify EGFR and co-occurring genetic alterations in tissue or plasma before and after SCLC transformation. Single-cell RNA sequencing (scRNA-seq) was performed on a patient-derived-xenograft model generated from a patient with EGFR-NSCLC transformed SCLC tumor.

Results

A total of 34 patients were identified in our study. Median age at initial diagnosis was 58, and median time to SCLC transformation was 24.2 months. 68% were female and 82% were never smokers. 79% of patients were diagnosed as stage IV disease, and over half had brain metastases at baseline. Median overall survival of the entire cohort was 38.3 months from initial diagnoses and 12.4 months from time of SCLC transformation. Most patients harbored EGFR exon19 deletions as opposed to exon21 L858R alteration. Continuing EGFR tyrosine kinase inhibitor post-transformation did not improve overall survival compared with those patients where tyrosine kinase inhibitor was stopped in our cohort. In the 20 paired pretransformed and post-transformed patient samples, statistically significant enrichment was seen with PIK3CA alterations (p = 0.04) post-transformation. Profiling of longitudinal liquid biopsy samples suggest emergence of SCLC genetic alterations before biopsy-proven SCLC, as shown by increasing variant allele frequency of TP53, RB1, PIK3CA alterations. ScRNA-seq revealed potential therapeutic targets including DLL3, CD276 (B7-H3) and PTK7 were widely expressed in transformed SCLC.

Conclusions

SCLC transformation is a potential treatment resistance mechanism in driver-mutant NSCLC. In our cohort of 34 EGFR-mutant NSCLC, poor prognosis was observed after SCLC transformation. Clinicogenomic analyses of paired and longitudinal samples identified genomic alterations emerging post-transformation and scRNA-seq reveal potential therapeutic targets in this population. Further studies are needed to rigorously validate biomarkers and therapeutic targets for this patient population.

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145
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19 weeks
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