Consensus molecular subtype transition during progression of colorectal cancer

IF 5.6 2区医学 Q1 ONCOLOGY

The Journal of Pathology Pub Date : 2023-09-08 DOI:10.1002/path.6176

Simone van de Weerd, Arezo Torang, Liselotte W Zwager, Pim J Koelink, Jan Koster, Barbara AJ Bastiaansen, Veerle Lammers, Ciro Longobardi, Jeanine ML Roodhart, J Han van Krieken, Arantza Farina Sarasqueta, Evelien Dekker, Jan Paul Medema

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Abstract

The consensus molecular subtype (CMS) classification divides colorectal cancer (CRC) into four distinct subtypes based on RNA expression profiles. The biological differences between CMSs are already present in CRC precursor lesions, but not all CMSs pose the same risk of malignant transformation. To fully understand the path to malignant transformation and to determine whether CMS is a fixed entity during progression, genomic and transcriptomic data from two regions of the same CRC lesion were compared: the precursor region and the carcinoma region. In total, 24 patients who underwent endoscopic removal of T1–2 CRC were included. Regions were subtyped for CMS and DNA mutation analysis was performed. Additionally, a set of 85 benign adenomas was CMS-subtyped. This analysis revealed that almost all benign adenomas were classified as CMS3 (91.8%). In contrast, CMS2 was the most prevalent subtype in precursor regions (66.7%), followed by CMS3 (29.2%). CMS4 was absent in precursor lesions and originated at the carcinoma stage. Importantly, CMS switching occurred in a substantial number of cases and almost all (six out of seven) CMS3 precursor regions showed a shift to a different subtype in the carcinoma part of the lesion, which in four cases was classified as CMS4. In conclusion, our data indicate that CMS3 is related to a more indolent type of precursor lesion that less likely progresses to CRC and when this occurs, it is often associated with a subtype change that includes the more aggressive mesenchymal CMS4. In contrast, an acquired CMS2 signature appeared to be rather fixed during early CRC development. Combined, our data show that subtype changes occur during progression and that CMS3 switching is related to changes in the genomic background through acquisition of a novel driver mutation (TP53) or selective expansion of a clone, but also occurred independently of such genetic changes. © 2023 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of The Pathological Society of Great Britain and Ireland.

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癌症进展过程中的一致分子亚型转变

共有分子亚型（CMS）分类根据RNA表达谱将癌症（CRC）分为四种不同的亚型。CMS之间的生物学差异已经存在于CRC前病变中，但并非所有CMS都具有相同的恶性转化风险。为了充分了解恶性转化的途径，并确定CMS在进展过程中是否是一个固定的实体，比较了同一CRC病变的两个区域的基因组和转录组数据：前体区域和癌区域。总共有24名患者接受了内镜下T1-2CRC切除术。对CMS的区域进行分型，并进行DNA突变分析。此外，一组85个良性腺瘤为CMS亚型。该分析显示，几乎所有良性腺瘤都被归类为CMS3（91.8%）。相反，CMS2是前驱区最常见的亚型（66.7%），其次是CMS3（29.2%）。CMS4在前驱病变中不存在，起源于癌症阶段。重要的是，CMS转换发生在大量病例中，几乎所有（七分之六）CMS3前体区域在病变的癌部分都显示出向不同亚型的转移，在四例病例中被归类为CMS4。总之，我们的数据表明，CMS3与一种更惰性的前体病变有关，这种病变不太可能发展为CRC，当这种情况发生时，它通常与亚型变化有关，其中包括更具侵袭性的间充质CMS4。相反，在CRC的早期发展过程中，获得的CMS2签名似乎是相当固定的。综合起来，我们的数据表明，亚型变化发生在进展过程中，CMS3转换与通过获得新的驱动突变（TP53）或克隆的选择性扩增而引起的基因组背景变化有关，但也独立于这种遗传变化而发生。©2023作者。病理学杂志由John Wiley&；代表大不列颠及爱尔兰病理学会的Sons有限公司。

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

The Journal of Pathology 医学-病理学

CiteScore

14.10

自引率

1.40%

发文量

144

审稿时长

3-8 weeks

期刊介绍： The Journal of Pathology aims to serve as a translational bridge between basic biomedical science and clinical medicine with particular emphasis on, but not restricted to, tissue based studies. The main interests of the Journal lie in publishing studies that further our understanding the pathophysiological and pathogenetic mechanisms of human disease. The Journal of Pathology welcomes investigative studies on human tissues, in vitro and in vivo experimental studies, and investigations based on animal models with a clear relevance to human disease, including transgenic systems. As well as original research papers, the Journal seeks to provide rapid publication in a variety of other formats, including editorials, review articles, commentaries and perspectives and other features, both contributed and solicited.