A Minimal Gene Set Characterizes TIL Specific for Diverse Tumor Antigens Across Different Cancer Types

Overview

Journal Nat Commun

Date 2025 Feb 3

PMID 39900903

Authors

Zhen Zeng

Tianbei Zhang

Jiajia Zhang

Shuai Li

Sydney Connor

Boyang Zhang

Yimin Zhao

Jordan Wilson

Dipika Singh

Rima Kulikauskas

Candice D Church

Thomas H Pulliam

Saumya Jani

Paul Nghiem

Suzanne L Topalian

Patrick M Forde

Drew M Pardoll

Hongkai Ji

Kellie N Smith

Affiliations

Soon will be listed here.

Abstract

Identifying tumor-specific T cell clones that mediate immunotherapy responses remains challenging. Mutation-associated neoantigen (MANA) -specific CD8+ tumor-infiltrating lymphocytes (TIL) have been shown to express high levels of CXCL13 and CD39 (ENTPD1), and low IL-7 receptor (IL7R) levels in many cancer types, but their collective relevance to T cell functionality has not been established. Here we present an integrative tool to identify MANA-specific TIL using weighted expression levels of these three genes in lung cancer and melanoma single-cell RNAseq datasets. Our three-gene "MANAscore" algorithm outperforms other RNAseq-based algorithms in identifying validated neoantigen-specific CD8+ clones, and accurately identifies TILs that recognize other classes of tumor antigens, including cancer testis antigens, endogenous retroviruses and viral oncogenes. Most of these TIL are characterized by a tissue resident memory gene expression program. Putative tumor-reactive cells (pTRC) identified via MANAscore in anti-PD-1-treated lung tumors had higher expression of checkpoint and cytotoxicity-related genes relative to putative non-tumor-reactive cells. pTRC in pathologically responding tumors showed distinguished gene expression patterns and trajectories. Collectively, we show that MANAscore is a robust tool that can greatly enrich candidate tumor-specific T cells and be used to understand the functional programming of tumor-reactive TIL.

Citing Articles

A minimal gene set characterizes TIL specific for diverse tumor antigens across different cancer types.

Zeng Z, Zhang T, Zhang J, Li S, Connor S, Zhang B Nat Commun. 2025; 16(1):1070.

PMID: 39900903 PMC: 11791090. DOI: 10.1038/s41467-024-55059-3.

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