澳大利亚人群中转移性结直肠癌的多基因检测二代测序
Multigene panel next generation sequencing in metastatic colorectal cancer in an Australian population.
作者信息
Nindra Udit, Pal Abhijit, Lea Vivienne, Lim Stephanie Hui-Su, Wilkinson Kate, Asghari Ray, Roberts Tara L, Becker Therese M, Farzin Mahtab, Rutland Tristan, Lee Mark, MacKenzie Scott, Ng Weng, Wang Bin, Lee C Soon, Chua Wei
机构信息
Department of Medical Oncology, Liverpool Hospital, Liverpool, New South Wales, Australia.
Department of Medical Oncology, Macarthur Cancer Therapy Centre, Campbelltown Hospital, Campbelltown, New South Wales, Australia.
出版信息
PLoS One. 2023 Oct 5;18(10):e0292087. doi: 10.1371/journal.pone.0292087. eCollection 2023.
BACKGROUND
Next generation sequencing (NGS) is increasingly used in standard clinical practice to identify patients with potentially actionable mutations. Stratification of NGS mutation tiers is currently based on the European Society of Medical Oncology (ESMO) Scale for Clinical Actionability of Molecular Targets (ESCAT[E]) Tier I-V & X. Allele frequency is also increasingly recognised as an important prognostic tool in advanced cancer. The aim of this study was to determine the genomic mutations in metastatic colorectal cancer (CRC) in an Australian multicultural population and their influence on survival outcomes.
METHODS
Next generation sequencing with the 50-gene panel Oncomine Precision Assay™ was used on 180 CRC tissue samples obtained across six Sydney hospitals between June 2021 and March 2022.
RESULTS
From 180 samples, 147 (82%) had at least one gene mutation identified with 68 (38%) having two or more concurrent mutations. Tier I variants included RAS wild-type [EI] in 73 (41%) and BRAF V600E [EIA] in 27 (15%). Non-tier I variants include 2 (1%) ERBB2 amplification [EIIB], 26 (15%) PIK3CA hotspot mutations [EIIIA] and 9 (5%) MET focal amplifications [EIIIA]. NGS testing revealed an additional 22% of cases with Tier II & III mutations. 43% of patients also presented with potentially actionable Tier III & IV mutations. Patients with concurrent TP53 and RAS mutations had significantly reduced overall survival (6.1 months versus 21.1 months, p <0.01). High KRAS allele frequency, as defined by those with over 20% variant allele frequency (VAF), also demonstrated reduced overall survival (12.1 months versus 42.9 months, p = 0.04).
CONCLUSIONS
In addition to identifying patients with genomic alterations suitable for clinically proven standard of care therapeutic options, the 50 gene NGS panel has significant potential in identifying potentially actionable non-tier 1 mutations and therefore may become future standard clinical practice.
背景
下一代测序(NGS)在标准临床实践中越来越多地用于识别具有潜在可操作突变的患者。目前,NGS突变层级的分层基于欧洲医学肿瘤学会(ESMO)分子靶点临床可操作性量表(ESCAT[E])的I-V级和X级。等位基因频率也越来越被认为是晚期癌症的一种重要预后工具。本研究的目的是确定澳大利亚多元文化人群中转移性结直肠癌(CRC)的基因组突变及其对生存结果的影响。
方法
2021年6月至2022年3月期间,在悉尼的六家医院采集了180份CRC组织样本,使用包含50个基因的Oncomine Precision Assay™进行下一代测序。
结果
在180份样本中,147份(82%)至少鉴定出一个基因突变,其中68份(38%)有两个或更多并发突变。I级变异包括73份(41%)RAS野生型[EI]和27份(15%)BRAF V600E[EIA]。非I级变异包括2份(1%)ERBB2扩增[EIIB]、26份(15%)PIK3CA热点突变[EIIIA]和9份(5%)MET局灶性扩增[EIIIA]。NGS检测发现另外22%的病例存在II级和III级突变。43%的患者还存在潜在可操作的III级和IV级突变。同时存在TP53和RAS突变的患者总生存期显著缩短(6.1个月对21.1个月,p<0.01)。以变异等位基因频率(VAF)超过20%定义的高KRAS等位基因频率也显示总生存期缩短(12.1个月对42.9个月,p=0.04)。
结论
除了识别具有适合临床验证的标准治疗选择的基因组改变的患者外,50基因NGS检测板在识别潜在可操作的非I级突变方面具有巨大潜力,因此可能成为未来的标准临床实践。
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