Single-cell transcriptomic analysis of normal and pathological tissues from the same patient uncovers colon cancer progression

Author:

Sun Ruifang,Yang YangORCID,Lü Weidong,Yang Yanqi,Li Yulong,Liu Zhigang,Diao Dongmei,Wang Yang,Chang Su’e,Lu Mengnan,Jiang Qiuyu,Dai Bingling,Ma Xiaobin,Zhao Chang’an,Lü Moqi,Zhang Juan,Ding Caixia,Li Na,Zhang Jian,Xiao Zhengtao,Zhou Dangxia,Huang Chen

Abstract

AbstractThe aim of the present study was to elucidate the evolutionary trajectory of colon cells from normal colon mucosa, to adenoma, then to carcinoma in the same microenvironment. Normal colon, adenoma and carcinoma tissues from the same patient were analyzed by single-cell sequencing, which perfectly simulated the process of time-dependent colon cancer due to the same microenvironment. A total of 22 cell types were identified. Results suggest the presence of dominant clones of same cells including C2 goblet cell, epithelial cell subtype 1 (Epi1), enterocyte cell subset 0 (Entero0), and Entero5 in carcinoma. Epi1 and Entero0 were Co-enriched in antibacterial and IL-17 signaling, Entero5 was enriched in immune response and mucin-type O-glycan biosynthesis. We discovered new colon cancer related genes including AC007952.4, NEK8, CHRM3, ANO7, B3GNT6, NEURL1, ODC1 and KCNMA1. The function of TBC1D4, LTB, C2CD4A, AND GBP4/5 in T cells needs to be clarified. We used colon samples from the same person, which provide new information for colon cancer therapy.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

Subject

General Biochemistry, Genetics and Molecular Biology

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