Skip to search boxSkip to navigationSkip to main content

Decoding hepatobiliary-specific immune gene patterns in gastrointestinal cancers via gene ontology fingerprints, multi-omics and experimental integration

  • Honglian Huan
    ,
  • Yueping Zhan
    ,
  • Hui Zong
    ,
  • Chenjun Huang
    ,
  • Fan Yang
    ,
  • Ziyi Wei
  • Tongji University
    ,
  • Shanghai University of Traditional Chinese Medicine
    ,
  • Heidelberg University 
    ,
  • Zhejiang University
    ,
  • University of Oxford
    ,
  • Shanxi University
Research Output: Contribution to journal Article Peer-review

Open access

Sustainable Development Goals

  • SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well

Abstract

Background Gastrointestinal (GI) cancers are characterized by high malignancy and poor prognosis. Tumors in different locations exhibit both commonalities and differences. Although immunotherapy has made progress in some GI cancers, the specific immune-related patterns in hepatobiliary tumors have not yet been fully elucidated. Methods Using our developed explainable gene ontology fingerprint (XGOF) method, GI cancer GOF was established. By integrating omics data from 20 hepatocellular carcinoma (HCC) and 15 cholangiocarcinoma (ICC) tissues in our clinic with public databases, immune-related patterns specifically expressed in hepatobiliary tumors were identified via RNA, protein, methylation, tumor microenvironment (TME) analysis and experimental verification. Results XGOF showed that GI cancers are related to diverse immune functions, especially macrophage migration. Compared to others, hepatobiliary tumors exhibit distinct patterns of gene expression, mutation, and methylation. Seven genes (APOA1, LBP, FGA, C9, APCS, ARG1 and MBL2) were identified as immune-related genes specifically decreased in hepatobiliary cancer. The impact of APOA1 on TME, prognosis, and genomic landscape in HCC was explored in prior research. In this work, the experiment confirmed the down-regulation of six genes in cancerous tissues. Moreover, LBP promoter methylation was elevated in cholangiocarcinoma. Single-cell analysis revealed downregulated immune genes in hepatocytes of HCC and cholangiocytes of ICC, enriched in humoral immunity and complement pathways. Additionally, the MIF pathway was identified as a key signal in interactions between ICC tumor cells and microenvironmental cells. Conclusion This study identified immune-related gene patterns in hepatobiliary cancer, contributing to the discovery of novel immunotherapy targets and tumor biomarkers for future research.

Publication Information

Output type

Research Output: Contribution to journal Article Peer-review

Original language

English

Article number

pbaf014

Journal (Volume, Issue Number)

Precision Clinical Medicine (Volume 8, Issue 3)

Publication milestones

  • Accepted/In press - 19/06/2025
  • Published - 24/06/2025

Publication status

Published - 24/06/2025

ISSN

2096-5303

External Publication IDs

  • handle.net: 10547/626710
  • Scopus: 105013051452
  • PubMed: 40657162

Publication metrics

Metrics

Download statistics
Download count
2

PlumX, opens in new tab

Social media
17
Captures
3
1
Mentions
10