Single-cell and bulk transcriptome sequencing identifies two epithelial tumor cell states and refines the consensus molecular classification of colorectal cancer

Author:

Joanito IgnasiusORCID,Wirapati PratyakshaORCID,Zhao NancyORCID,Nawaz ZahidORCID,Yeo GraceORCID,Lee FionaORCID,Eng Christine L. P.,Macalinao Dominique Camat,Kahraman Merve,Srinivasan Harini,Lakshmanan Vairavan,Verbandt Sara,Tsantoulis PetrosORCID,Gunn Nicole,Venkatesh Prasanna NoriORCID,Poh Zhong Wee,Nahar Rahul,Oh Hsueh Ling Janice,Loo Jia MinORCID,Chia Shumei,Cheow Lih Feng,Cheruba ElsieORCID,Wong Michael Thomas,Kua LindsayORCID,Chua Clarinda,Nguyen AndyORCID,Golovan Justin,Gan Anna,Lim Wan-Jun,Guo Yu AmandaORCID,Yap Choon Kong,Tay Brenda,Hong YouraeORCID,Chong Dawn Qingqing,Chok Aik-Yong,Park Woong-Yang,Han Shuting,Chang Mei Huan,Seow-En IsaacORCID,Fu Cherylin,Mathew Ronnie,Toh Ee-LinORCID,Hong Lewis Z.ORCID,Skanderup Anders JacobsenORCID,DasGupta RamanujORCID,Ong Chin-Ann Johnny,Lim Kiat Hon,Tan Emile K. W.,Koo Si-Lin,Leow Wei Qiang,Tejpar SabineORCID,Prabhakar ShyamORCID,Tan Iain BeehuatORCID

Abstract

AbstractThe consensus molecular subtype (CMS) classification of colorectal cancer is based on bulk transcriptomics. The underlying epithelial cell diversity remains unclear. We analyzed 373,058 single-cell transcriptomes from 63 patients, focusing on 49,155 epithelial cells. We identified a pervasive genetic and transcriptomic dichotomy of malignant cells, based on distinct gene expression, DNA copy number and gene regulatory network. We recapitulated these subtypes in bulk transcriptomes from 3,614 patients. The two intrinsic subtypes, iCMS2 and iCMS3, refine CMS. iCMS3 comprises microsatellite unstable (MSI-H) cancers and one-third of microsatellite-stable (MSS) tumors. iCMS3 MSS cancers are transcriptomically more similar to MSI-H cancers than to other MSS cancers. CMS4 cancers had either iCMS2 or iCMS3 epithelium; the latter had the worst prognosis. We defined the intrinsic epithelial axis of colorectal cancer and propose a refined ‘IMF’ classification with five subtypes, combining intrinsic epithelial subtype (I), microsatellite instability status (M) and fibrosis (F).

Publisher

Springer Science and Business Media LLC

Subject

Genetics

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