An invasive zone in human liver cancer identified by Stereo-seq promotes hepatocyte–tumor cell crosstalk, local immunosuppression and tumor progression

Liang Wu; Jiayan Yan; Yinqi Bai; Feiyu Chen; Xuanxuan Zou; Jiangshan Xu; Ao Huang; Liangzhen Hou; Yu Zhong; Zehua Jing; Qichao Yu; Xiaorui Zhou; Zhifeng Jiang; Chunqing Wang; Mengnan Cheng; Yuan Ji; Yingyong Hou; Rongkui Luo; Qinqin Li; Liang Wu; Jianwen Cheng; Pengxiang Wang; De‐Zhen Guo; Waidong Huang; Junjie Lei; Shang Liu; Yizhen Yan; Yi‐Ling Chen; Sha Liao; Yuxiang Li; Haixiang Sun; Na Yao; Xiangyu Zhang; Shiyu Zhang; Xi Chen; Yang Yu; Yao Li; Fengming Liu; Zheng Wang; Shao‐Lai Zhou; Huanming Yang; Shuang Yang; Xun Xu; Longqi Liu; Qiang Gao; Zhao–You Tang; Xiangdong Wang; Jian Wang; Jia Fan; Shiping Liu; Xin‐Rong Yang; Ao Chen; Jian Zhou

doi:10.1038/s41422-023-00831-1

An invasive zone in human liver cancer identified by Stereo-seq promotes hepatocyte–tumor cell crosstalk, local immunosuppression and tumor progression

Liang Wu(BGI Group (China)), Jiayan Yan(Fudan University), Yinqi Bai(Fudan University), Feiyu Chen(Fudan University), Xuanxuan Zou(BGI Group (China)), Jiangshan Xu(University of Chinese Academy of Sciences), Ao Huang(Fudan University), Liangzhen Hou(University of Chinese Academy of Sciences), Yu Zhong, Zehua Jing(University of Chinese Academy of Sciences), Qichao Yu(University of Chinese Academy of Sciences), Xiaorui Zhou(University of Chinese Academy of Sciences), Zhifeng Jiang(Fudan University), Chunqing Wang(University of Chinese Academy of Sciences), Mengnan Cheng(University of Chinese Academy of Sciences), Yuan Ji(Sun Yat-sen University), Yingyong Hou(Sun Yat-sen University), Rongkui Luo(Sun Yat-sen University), Qinqin Li(Shanghai Jiao Tong University), Liang Wu(BGI Group (China)), Jianwen Cheng(Fudan University), Pengxiang Wang(Fudan University), De‐Zhen Guo(Fudan University), Waidong Huang(University of Chinese Academy of Sciences), Junjie Lei(University of Chinese Academy of Sciences), Shang Liu(Shenzhen University), Yizhen Yan, Yi‐Ling Chen, Sha Liao(BGI Group (China)), Yuxiang Li(Chinese Academy of Sciences), Haixiang Sun(Fudan University), Na Yao(Fudan University), Xiangyu Zhang(Fudan University), Shiyu Zhang(Fudan University), Xi Chen, Yang Yu(Chinese Academy of Sciences), Yao Li(Chinese Academy of Sciences), Fengming Liu(Chinese Academy of Sciences), Zheng Wang(Fudan University), Shao‐Lai Zhou(Fudan University), Huanming Yang, Shuang Yang(Fudan University), Xun Xu(Fudan University), Longqi Liu(Fudan University), Qiang Gao(Fudan University), Zhao–You Tang(Fudan University), Xiangdong Wang(Fudan University), Jian Wang(Fudan University), Jia Fan(Fudan University), Shiping Liu(BGI Group (China)), Xin‐Rong Yang(Fudan University), Ao Chen(BGI Group (China)), Jian Zhou(Fudan University)

Cell Research

June 19, 2023

10.1038/s41422-023-00831-1

Cited by 211Open Access

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Abstract

Abstract Dissecting and understanding the cancer ecosystem, especially that around the tumor margins, which have strong implications for tumor cell infiltration and invasion, are essential for exploring the mechanisms of tumor metastasis and developing effective new treatments. Using a novel tumor border scanning and digitization model enabled by nanoscale resolution-SpaTial Enhanced REsolution Omics-sequencing (Stereo-seq), we identified a 500 µm-wide zone centered around the tumor border in patients with liver cancer, referred to as “the invasive zone”. We detected strong immunosuppression, metabolic reprogramming, and severely damaged hepatocytes in this zone. We also identified a subpopulation of damaged hepatocytes with increased expression of serum amyloid A1 and A2 (referred to collectively as SAAs) located close to the border on the paratumor side. Overexpression of CXCL6 in adjacent malignant cells could induce activation of the JAK-STAT3 pathway in nearby hepatocytes, which subsequently caused SAAs’ overexpression in these hepatocytes. Furthermore, overexpression and secretion of SAAs by hepatocytes in the invasive zone could lead to the recruitment of macrophages and M2 polarization, further promoting local immunosuppression, potentially resulting in tumor progression. Clinical association analysis in additional five independent cohorts of patients with primary and secondary liver cancer ( n = 423) showed that patients with overexpression of SAAs in the invasive zone had a worse prognosis. Further in vivo experiments using mouse liver tumor models in situ confirmed that the knockdown of genes encoding SAAs in hepatocytes decreased macrophage accumulation around the tumor border and delayed tumor growth. The identification and characterization of a novel invasive zone in human cancer patients not only add an important layer of understanding regarding the mechanisms of tumor invasion and metastasis, but may also pave the way for developing novel therapeutic strategies for advanced liver cancer and other solid tumors.

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