3D genome landscape of primary and metastatic colorectal carcinoma reveals the regulatory mechanism of tumorigenic and metastatic gene expression.

IF 5.1 1区 生物学 Q1 BIOLOGY Communications Biology Pub Date : 2025-03-04 DOI:10.1038/s42003-025-07647-2
Xiang Xu, Jingbo Gan, Zhaoya Gao, Ruifeng Li, Dandan Huang, Lin Lin, Yawen Luo, Qian Yang, Jingxuan Xu, Yaru Li, Qing Fang, Ting Peng, Yaqi Wang, Zihan Xu, An Huang, Haopeng Hong, Fuming Lei, Wensheng Huang, Jianjun Leng, Tingting Li, Xiaochen Bo, Hebing Chen, Cheng Li, Jin Gu
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Abstract

Colorectal carcinoma (CRC) is a deadly cancer with an aggressive nature, and how CRC tumor cells manage to translocate and proliferate in a new tissue environment remains not fully understood. Recently, higher-order chromatin structures and spatial genome organization are increasingly implicated in diseases including cancer, but in-depth studies of three-dimensional genome (3D genome) of metastatic cancer are currently lacking, preventing the understanding of the roles of genome organization during metastasis. Here we perform multi-omics profiling of matched normal colon, primary tumor, lymph node metastasis, liver metastasis and normal liver tissue from CRC patients using Hi-C, ATAC-seq and RNA-seq technologies. We find that widespread alteration of 3D chromatin structure is accompanied by dysregulation of genes including SPP1 during the tumorigenesis or metastasis of CRC. Remarkably, the hierarchy of topological associating domain (TAD) changes dynamically, which challenges the traditional view that the TAD structure between tumor and normal tissue is conservative. In addition, we define compartment stability score to measure large-scale alteration in metastatic tumors. To integrate multi-omics data and recognize candidate genes driving cancer metastasis, a pipeline is developed based on Hi-C, RNA-seq and ATAC-seq data. And three candidate genes ARL4C, FLNA, and RGCC are validated to be associated with CRC cell migration and invasion using in vitro knockout experiments. Overall, these data resources and results offer new insights into the involvement of 3D genome in cancer metastasis.

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原发性和转移性结直肠癌的三维基因组图谱揭示了致瘤性和转移性基因表达的调控机制。
结直肠癌(CRC)是一种具有侵袭性的致命癌症,CRC肿瘤细胞如何在新的组织环境中转移和增殖尚不完全清楚。近年来,高阶染色质结构和空间基因组组织越来越多地与包括癌症在内的疾病有关,但目前缺乏对转移性癌症的三维基因组(3D基因组)的深入研究,阻碍了对基因组组织在转移过程中的作用的理解。本研究采用Hi-C、ATAC-seq和RNA-seq技术对结直肠癌患者的正常结肠、原发肿瘤、淋巴结转移、肝转移和正常肝组织进行多组学分析。我们发现,在结直肠癌的肿瘤发生或转移过程中,三维染色质结构的广泛改变伴随着包括SPP1在内的基因的失调。值得注意的是,拓扑关联域(TAD)的层次结构是动态变化的,这挑战了传统观点,即肿瘤与正常组织之间的TAD结构是保守的。此外,我们定义了室稳定性评分来衡量转移性肿瘤的大规模改变。为了整合多组学数据并识别驱动肿瘤转移的候选基因,基于Hi-C、RNA-seq和ATAC-seq数据建立了一个管道。通过体外敲除实验验证了三个候选基因ARL4C、FLNA和RGCC与结直肠癌细胞迁移和侵袭相关。总的来说,这些数据资源和结果为3D基因组参与癌症转移提供了新的见解。
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
Communications Biology
Communications Biology Medicine-Medicine (miscellaneous)
CiteScore
8.60
自引率
1.70%
发文量
1233
审稿时长
13 weeks
期刊介绍: Communications Biology is an open access journal from Nature Research publishing high-quality research, reviews and commentary in all areas of the biological sciences. Research papers published by the journal represent significant advances bringing new biological insight to a specialized area of research.
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