实时靶向胰腺导管腺癌基因组分析鉴定可能靶向现有药物或用作生物标志物的遗传改变。
Real-Time Targeted Genome Profile Analysis of Pancreatic Ductal Adenocarcinomas Identifies Genetic Alterations That Might Be Targeted With Existing Drugs or Used as Biomarkers.
机构信息
Department of Pathology, University of Pittsburgh Medical Center, Pittsburgh, Pennsylvania.
Department of Medicine, Division of Medical Oncology, Medical College of Wisconsin, Milwaukee, Wisconsin.
出版信息
Gastroenterology. 2019 Jun;156(8):2242-2253.e4. doi: 10.1053/j.gastro.2019.02.037. Epub 2019 Mar 2.
BACKGROUND & AIMS: It has been a challenge to select treatment for patients with pancreatic ductal adenocarcinomas (PDACs) based on genome alterations. We performed targeted genomic profile analyses of a large number of PDACs to assess the full spectrum of actionable genomic alterations.
METHODS
We performed targeted genomic profile analyses of 3594 PDAC samples from an international cohort, including capture-based targeted genomic profiling of as many as 315 cancer-associated genes and intron regions of 28 genes that are rearranged in cancer cells. Tumor mutation burden (TMB) and microsatellite instability (MSI) status were also assessed. TMB was calculated across a 1.14-megabase region; TMB-high was defined as ≥20 mutations/megabase. MSI-high status was assigned based on analysis of 114 intron homopolymer loci.
RESULTS
KRAS, TP53, CDKN2A, and SMAD4 were the most frequently altered genes in PDAC. We found KRAS mutations in 88% of samples. Among PDACs without mutations in KRAS, we found alterations in genes whose products are in the mitogen-activated protein kinase signaling pathway and are candidate drug targets (actionable targets, n = 132; 4%), as well as gene fusions (n = 51), gene amplifications (n = 35), genes with missense mutations (n = 30), and genes that contain deletions (n = 16). Many of these encode proteins in receptor tyrosine kinase, RAS, or mitogen-activated protein kinase signaling pathways. Aside from TP53, alterations in genes encoding DNA damage repair proteins (BRCA and FANC) were detected in 14% of PDACs. Among PDACs evaluated for MSI (n = 2563) and TMB (n = 1021), MSI-high and/or TMB-high phenotypes were detected in 0.5% of samples. Alterations in FGF23, CCND2, PIK3CA, and FGF6 were more commonly detected in intraductal papillary mucinous neoplasm-associated PDACs.
CONCLUSIONS
In targeted genomic profile analyses of 3594 PDACs, we found 17% to contain genomic alterations that might make the tumor cells susceptible to currently used anticancer agents. We identified mutations in genes that could contribute to progression of intraductal papillary mucinous neoplasms into malignancies. These alterations might be used as biomarkers for early detection.
背景与目的
根据基因组改变选择治疗胰腺导管腺癌(PDAC)患者一直是一个挑战。我们对大量 PDAC 进行了靶向基因组谱分析,以评估全谱可操作的基因组改变。
方法
我们对来自国际队列的 3594 例 PDAC 样本进行了靶向基因组谱分析,包括多达 315 个癌症相关基因和在癌细胞中重排的 28 个基因的内含子区域的基于捕获的靶向基因组谱分析。还评估了肿瘤突变负担(TMB)和微卫星不稳定性(MSI)状态。TMB 是在 1.14 兆碱基区域计算的;TMB 高定义为≥20 个突变/兆碱基。MSI 高状态是基于对 114 个内含子同源多聚体位点的分析确定的。
结果
KRAS、TP53、CDKN2A 和 SMAD4 是 PDAC 中最常改变的基因。我们在 88%的样本中发现了 KRAS 突变。在没有 KRAS 突变的 PDAC 中,我们发现了其产物存在于丝裂原活化蛋白激酶信号通路中的基因改变,并且是候选药物靶点(可操作靶点,n=132;4%),以及基因融合(n=51)、基因扩增(n=35)、错义突变基因(n=30)和包含缺失的基因(n=16)。其中许多基因编码受体酪氨酸激酶、RAS 或丝裂原活化蛋白激酶信号通路中的蛋白质。除了 TP53 之外,在 14%的 PDAC 中还检测到编码 DNA 损伤修复蛋白(BRCA 和 FANC)的基因改变。在评估 MSI(n=2563)和 TMB(n=1021)的 PDAC 中,在 0.5%的样本中检测到 MSI 高和/或 TMB 高表型。在与导管内乳头状黏液性肿瘤相关的 PDAC 中,更常检测到 FGF23、CCND2、PIK3CA 和 FGF6 的改变。
结论
在对 3594 例 PDAC 的靶向基因组谱分析中,我们发现 17%的肿瘤含有可能使肿瘤细胞对现有抗癌药物敏感的基因组改变。我们发现了可能导致导管内乳头状黏液性肿瘤进展为恶性肿瘤的基因突变。这些改变可能可作为早期检测的生物标志物。
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