种系EGFR突变与家族性癌症。

IF 42.1 1区 医学 Q1 ONCOLOGY Journal of Clinical Oncology Pub Date : 2023-12-01 Epub Date: 2023-10-23 DOI:10.1200/JCO.23.01372
Geoffrey R Oxnard, Ruthia Chen, Jennifer C Pharr, Diane R Koeller, Arrien A Bertram, Suzanne E Dahlberg, Irene Rainville, Kate Shane-Carson, Kelly A Taylor, Alicia Sable-Hunt, Lynette M Sholl, Craig C Teerlink, Alun Thomas, Lisa A Cannon-Albright, André P Fay, Patrícia Ashton-Prolla, Hao Yang, Mary M Salvatore, Bonnie J Addario, Pasi A Jänne, David P Carbone, Georgia L Wiesner, Judy E Garber
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引用次数: 0

摘要

目的:遗传性癌症风险的基因组基础尚不清楚。这项前瞻性研究对具有种系EGFR致病性变体(PV)的患者和家庭的临床表型进行了表征。方法:T790M研究的遗传风险调查(ClinicalTrials.gov标识符:NCT01754025)招募了癌症患者及其亲属,这些患者的肿瘤特征包含可能的种系EGFR-PV,提供种系检测和随访。结果:在5年的时间里,共有141名参与者参与,其中100人(71%)远程参与。基于先前的基因分型,来自59个家族的116名参与者接受了EGFR T790M检测,证明了具有可变肺癌癌症外显率的孟德尔遗传模式。来自39个不同家族的种系EGFR PV的确诊或专性携带者中,50/91(55%)患上了癌症,其中34/65(52%)在60岁时被诊断为肺癌。对携带者肺癌的体细胞测试显示,37人中有35人(95%)患有EGFR驱动基因突变。在36名未被诊断为癌症的种系携带者中,15人进行了计算机断层扫描(CT)成像,9人有肺结节,其中包括一名28岁的肺结节>10。考虑到种系EGFR T790M在美国东南部的地理富集,对46个种系携带者进行了全基因组单倍型分析,确定了41个(89%)共享的4.1-Mb单倍型,估计起源于223-279年前。结论:据我们所知,这是家族性EGFR突变型癌症的首次前瞻性描述,鉴定了一种在美国东南部富集的最新创始人种系EGFR T790M变体。在种系携带者中,EGFR驱动的肺腺癌和肺结节的高患病率支持识别受影响的患者和家庭成员,以便对这些高危个体进行基于CT的筛查。
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Germline EGFR Mutations and Familial Lung Cancer.

Purpose: The genomic underpinnings of inherited lung cancer risk are poorly understood. This prospective study characterized the clinical phenotype of patients and families with germline EGFR pathogenic variants (PVs).

Methods: The Investigating Hereditary Risk from T790M study (ClinicalTrials.gov identifier: NCT01754025) enrolled patients with lung cancer whose tumor profiling harbored possible germline EGFR PVs and their relatives, either in person or remotely, providing germline testing and follow-up.

Results: A total of 141 participants were enrolled over a 5-year period, 100 (71%) remotely. Based upon previous genotyping, 116 participants from 59 kindreds were tested for EGFR T790M, demonstrating a pattern of Mendelian inheritance with variable lung cancer penetrance. In confirmed or obligate carriers of a germline EGFR PV from 39 different kindreds, 50/91 (55%) were affected with lung cancer with 34/65 (52%) diagnosed by age 60 years. Somatic testing of lung cancers in carriers revealed that 35 of 37 (95%) had an EGFR driver comutation. Among 36 germline carriers without a cancer diagnosis, 15 had computed tomography (CT) imaging and nine had lung nodules, including a 28-year-old with >10 lung nodules. Given geographic enrichment of germline EGFR T790M in the southeast United States, genome-wide haplotyping of 46 germline carriers was performed and identified a 4.1-Mb haplotype shared by 41 (89%), estimated to originate 223-279 years ago.

Conclusion: To our knowledge, this is the first prospective description of familial EGFR-mutant lung cancer, identifying a recent founder germline EGFR T790M variant enriched in the Southeast United States. The high prevalence of EGFR-driver lung adenocarcinomas and lung nodules in germline carriers supports effort to identify affected patients and family members for investigation of CT-based screening for these high-risk individuals.

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来源期刊
Journal of Clinical Oncology
Journal of Clinical Oncology 医学-肿瘤学
CiteScore
41.20
自引率
2.20%
发文量
8215
审稿时长
2 months
期刊介绍: The Journal of Clinical Oncology serves its readers as the single most credible, authoritative resource for disseminating significant clinical oncology research. In print and in electronic format, JCO strives to publish the highest quality articles dedicated to clinical research. Original Reports remain the focus of JCO, but this scientific communication is enhanced by appropriately selected Editorials, Commentaries, Reviews, and other work that relate to the care of patients with cancer.
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