Epigenome signature as an immunophenotype indicator prompts durable clinical immunotherapy benefits in lung adenocarcinoma

Xu Pan; Caiyu Zhang; Junwei Wang; Peng Wang; Yue Gao; Shipeng Shang; Shuang Guo; Xin Li; Hui Zhi; Shangwei Ning

doi:10.1093/bib/bbab481

Epigenome signature as an immunophenotype indicator prompts durable clinical immunotherapy benefits in lung adenocarcinoma

Brief Bioinform. 2022 Jan 17;23(1):bbab481. doi: 10.1093/bib/bbab481.

Authors

Xu Pan¹, Caiyu Zhang¹, Junwei Wang², Peng Wang¹, Yue Gao¹, Shipeng Shang¹, Shuang Guo¹, Xin Li^{1

3}, Hui Zhi¹, Shangwei Ning¹

Affiliations

¹ College of Bioinformatics Science and Technology, Harbin Medical University, Harbin 150081, China.
² Department of Respiratory Medicine, The Second Affiliated Hospital of Harbin Medical University, Harbin 150081, China.
³ Department of Dermatology, Xiangya Hospital, Central South University, Changsha 410008, China.

PMID: 34864866
DOI: 10.1093/bib/bbab481

Abstract

Intertumoral immune heterogeneity is a critical reason for distinct clinical benefits of immunotherapy in lung adenocarcinoma (LUAD). Tumor immunophenotype (immune 'Hot' or 'Cold') suggests immunological individual differences and potential clinical treatment guidelines. However, employing epigenome signatures to determine tumor immunophenotypes and responsive treatment is not well understood. To delineate the tumor immunophenotype and immune heterogeneity, we first distinguished the immune 'Hot' and 'Cold' tumors of LUAD based on five immune expression signatures. In terms of clinical presentation, the immune 'Hot' tumors usually had higher immunoactivity, lower disease stages and better survival outcomes than 'Cold' tumors. At the epigenome levels, we observed that distinct DNA methylation patterns between immunophenotypes were closely associated with LUAD development. Hence, we identified a set of five CpG sites as the immunophenotype-related methylation signature (iPMS) for tumor immunophenotyping and further confirmed its efficiency based on a machine learning framework. Furthermore, we found iPMS and immunophenotype-related immune checkpoints (IPCPs) could contribute to the risk of tumor progression, implying IPCP has the potential to be a novel immunotherapy blockade target. After further parsing of the role of iPMS-predicted immunophenotypes, we found immune 'Hot' was a protective factor leading to better survival outcomes when patients received the anti-PD-1/PD-L1 immunotherapy. And iPMS was also a well-performed signature (AUC = 0.752) for predicting the durable/nondurable clinical benefits. In summary, our study explored the role of epigenome signature in clinical tumor immunophenotyping. Utilizing iPMS to characterize tumor immunophenotypes will facilitate developing personalized epigenetic anticancer approaches.

Keywords: DNA methylation; anti-PD-1/PD-L1 immunotherapy; lung adenocarcinoma; personalized clinical treatment strategy; tumor immunophenotype.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenocarcinoma of Lung* / genetics
Adenocarcinoma of Lung* / therapy
Biomarkers, Tumor / genetics
Epigenome
Humans
Immunophenotyping
Immunotherapy
Lung Neoplasms* / drug therapy
Lung Neoplasms* / therapy

Substances

Biomarkers, Tumor