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Liver metastases across cancer types sharing tumor environment immunotolerance can impede immune response therapy and immune monitoring.

Authors :
Gao, Yuzhen
Chen, Shipeng
Wang, Hao
Wu, Chenghao
An, Rui
Li, Guoli
Yang, Min
Zhou, Ying
Zhou, Yundong
Xie, Xinyou
Yu, Hong
Zhang, Jun
Source :
Journal of Advanced Research. Jul2024, Vol. 61, p151-164. 14p.
Publication Year :
2024

Abstract

[Display omitted] • The prognosis of patients with liver metastasis is worse than that of other metastatic cancers across cancer types. • Part of patients with liver metastasis have common tumor environment immunotolerance. • The immunotolerance with low immune cells expression contributed the main features of liver metastasis across cancer types. • Liver metastasis common features score guides immunotherapy/prognosis of liver metastasis, with KRT19 playing a key role. Hepatic immune tolerance might contribute to the development of therapeutic resistance to immunotherapy. However, addressing this issue is challenging since the efficacy of immunotherapy in the context of liver metastasis (LM) remains poorly studied. Here, we aimed to establish an LM common immune feature (LMCIF) score to quantify the characteristics of LM immunotolerance across cancer types for assisting clinical disease management. Large-scale clinical data were collected to identify the prognosis of LM. Multi-omics datasets of metastatic cancers with LM special immune-related pathways (LMSIPs) from the Molecular Signatures Database (MSigDB) were used to obtain an LMCIF cluster. Based on differential expression genes (DEGs), a novel LMCIF score for the LMCIF cluster was constructed. In addition, multi-omics, and immunohistochemistry (IHC) data from the public and in-house cohorts were used to explore the features of LM, and LMCIF score. Patients with LM had a worse prognosis and significantly lower infiltration of immune cells than patients with metastasis to other organs when analyzed with combined clinical and RNA sequencing data. After extracting the LMCIF cluster from 373 samples by utilizing 29 LMSIPs and validating them in a microarray cohort, an LMCIF score was established to confirm the role of the immunosuppressive environment as a contributor to the poor prognosis of LM across cancer types. Moreover, this LMCIF score could be used to predict the immune response of cancer patients undergoing immunotherapy. Finally, we identified that the majority of the 31 LMCIF genes exhibited a negative correlation with TME cells in LM patients, one of them, KRT19, which possessed the strongest positive correlation with LMCIF score, was confirmed to have an immunosuppressive effect through IHC analysis. Our results suggest that LM across cancer types share similar immunological profiles that induce immunotolerance and escape from immune monitoring. The novel LMCIF score represents a common liver metastasis immune cluster for predicting immunotherapy response, the results of which might benefit clinical disease management. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
20901232
Volume :
61
Database :
Academic Search Index
Journal :
Journal of Advanced Research
Publication Type :
Academic Journal
Accession number :
178022096
Full Text :
https://doi.org/10.1016/j.jare.2023.08.011