Spatial intra-tumour heterogeneity and treatment-induced genomic evolution in oesophageal adenocarcinoma: implications for prognosis and therapy.

IF 10.4 1区 生物学 Q1 GENETICS & HEREDITY
Sandra Brosda, Lauren G Aoude, Vanessa F Bonazzi, Kalpana Patel, James M Lonie, Clemence J Belle, Felicity Newell, Lambros T Koufariotis, Venkateswar Addala, Marjan M Naeini, John V Pearson, Lutz Krause, Nicola Waddell, Andrew P Barbour
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引用次数: 0

Abstract

Background: Oesophageal adenocarcinoma (OAC) is a highly heterogeneous cancer with poor survival. Standard curative treatment is chemotherapy with or without radiotherapy followed by oesophagectomy. Genomic heterogeneity is a feature of OAC and has been linked to treatment resistance.

Methods: Whole-genome sequencing data from 59 treatment-naïve and 18 post-treatment samples from 29 OAC patients was analysed. Twenty-seven of these were enrolled in the DOCTOR trial, sponsored by the Australasian Gastro-Intestinal Trials Group. Two biopsies from each treatment-naïve tumour were assessed to define 'shared' (between both samples) and 'private' (present in one sample) mutations.

Results: Mutational signatures SBS2/13 (APOBEC) and SBS3 (BRCA) were almost exclusively detected in private mutation populations of treatment-naïve tumours. Patients presenting these signatures had significantly worse disease specific survival. Furthermore, mutational signatures associated with platinum-based chemotherapy treatment as well as high platinum enrichment scores were only detected in post-treatment samples. Additionally, clones with high putative neoantigen binding scores were detected in some treatment-naïve samples suggesting immunoediting of clones.

Conclusions: This study demonstrates the high intra-tumour heterogeneity in OAC, as well as indicators for treatment-induced changes during tumour evolution. Intra-tumour heterogeneity remains a problem for successful treatment strategies in OAC.

食管腺癌的瘤内空间异质性和治疗诱导的基因组演变:对预后和治疗的影响。
背景:食管腺癌(OAC)是一种高度异质性癌症,生存率很低。标准的根治性治疗是化疗加或不加放疗,然后进行食管切除术。基因组异质性是食管腺癌的一个特征,与耐药性有关:方法:分析了来自 29 名 OAC 患者的 59 份治疗前样本和 18 份治疗后样本的全基因组测序数据。其中 27 人参加了由澳大拉西亚胃肠道试验小组(Australasian Gastro-Intestinal Trials Group)赞助的 DOCTOR 试验。对每个治疗无效肿瘤的两个活检样本进行了评估,以确定 "共享"(两个样本之间)和 "私有"(存在于一个样本中)突变:结果:SBS2/13(APOBEC)和SBS3(BRCA)突变特征几乎全部在治疗无效肿瘤的私人突变群体中被检测到。出现这些特征的患者的疾病特异性生存率明显降低。此外,只有在治疗后样本中才能检测到与铂类化疗相关的突变特征以及高铂类富集分数。此外,在一些未经治疗的样本中检测到了具有高推定新抗原结合得分的克隆,这表明克隆存在免疫编辑:这项研究证明了 OAC 肿瘤内部的高度异质性,以及肿瘤演变过程中治疗诱导变化的指标。肿瘤内异质性仍然是OAC成功治疗策略的一个难题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Genome Medicine
Genome Medicine GENETICS & HEREDITY-
CiteScore
20.80
自引率
0.80%
发文量
128
审稿时长
6-12 weeks
期刊介绍: Genome Medicine is an open access journal that publishes outstanding research applying genetics, genomics, and multi-omics to understand, diagnose, and treat disease. Bridging basic science and clinical research, it covers areas such as cancer genomics, immuno-oncology, immunogenomics, infectious disease, microbiome, neurogenomics, systems medicine, clinical genomics, gene therapies, precision medicine, and clinical trials. The journal publishes original research, methods, software, and reviews to serve authors and promote broad interest and importance in the field.
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