Single-cell analysis reveals cellular and molecular factors counteracting HPV-positive oropharyngeal cancer immunotherapy outcomes

Junha Cha; Da Hee Kim; Gamin Kim; Jae-Won Cho; Euijeong Sung; Seungbyn Baek; Min Hee Hong; Chang Gon Kim; Nam Suk Sim; Hyun Jun Hong; Jung Eun Lee; Martin Hemberg; Seyeon Park; Sun Ock Yoon; Sang-Jun Ha; Yoon Woo Koh; Hye Ryun Kim; Insuk Lee

doi:10.1136/jitc-2023-008667

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Single-cell analysis reveals cellular and molecular factors counteracting HPV-positive oropharyngeal cancer immunotherapy outcomes

Authors: Junha Cha ; Da Hee Kim ; Gamin Kim ; Jae-Won Cho ; Euijeong Sung ; Seungbyn Baek ; Min Hee Hong ; Chang Gon Kim ; Nam Suk Sim ; Hyun Jun Hong ; Jung Eun Lee ; Martin Hemberg ; Seyeon Park ; Sun Ock Yoon ; Sang-Jun Ha ; Yoon Woo Koh ; Hye Ryun Kim ; Insuk Lee

Citation: JOURNAL FOR IMMUNOTHERAPY OF CANCER, Vol.12(6) : e008667, 2024-06

Journal Title: JOURNAL FOR IMMUNOTHERAPY OF CANCER

Issue Date: 2024-06

MeSH: Aged ; Female ; Humans ; Immunotherapy* / methods ; Male ; Middle Aged ; NK Cell Lectin-Like Receptor Subfamily B ; Oropharyngeal Neoplasms* / immunology ; Oropharyngeal Neoplasms* / therapy ; Oropharyngeal Neoplasms* / virology ; Papillomavirus Infections* / immunology ; Papillomavirus Infections* / virology ; Single-Cell Analysis*

Keywords: Head and Neck Cancer ; Immune Checkpoint Inhibitor ; Immunotherapy ; Tumor microenvironment - TME ; co-inhibitory molecule

Abstract: BACKGROUND: Oropharyngeal squamous cell carcinoma (OPSCC) induced by human papillomavirus (HPV-positive) is associated with better clinical outcomes than HPV-negative OPSCC. However, the clinical benefits of immunotherapy in patients with HPV-positive OPSCC remain unclear. METHODS: To identify the cellular and molecular factors that limited the benefits associated with HPV in OPSCC immunotherapy, we performed single-cell RNA (n=20) and T-cell receptor sequencing (n=10) analyses of tonsil or base of tongue tumor biopsies prior to immunotherapy. Primary findings from our single-cell analysis were confirmed through immunofluorescence experiments, and secondary validation analysis were performed via publicly available transcriptomics data sets. RESULTS: We found significantly higher transcriptional diversity of malignant cells among non-responders to immunotherapy, regardless of HPV infection status. We also observed a significantly larger proportion of CD4+ follicular helper T cells (Tfh) in HPV-positive tumors, potentially due to enhanced Tfh differentiation. Most importantly, CD8+ resident memory T cells (Trm) with elevated KLRB1 (encoding CD161) expression showed an association with dampened antitumor activity in patients with HPV-positive OPSCC, which may explain their heterogeneous clinical outcomes. Notably, all HPV-positive patients, whose Trm presented elevated KLRB1 levels, showed low expression of CLEC2D (encoding the CD161 ligand) in B cells, which may reduce tertiary lymphoid structure activity. Immunofluorescence of HPV-positive tumors treated with immune checkpoint blockade showed an inverse correlation between the density of CD161+ Trm and changes in tumor size. CONCLUSIONS: We found that CD161+ Trm counteracts clinical benefits associated with HPV in OPSCC immunotherapy. This suggests that targeted inhibition of CD161 in Trm could enhance the efficacy of immunotherapy in HPV-positive oropharyngeal cancers. TRIAL REGISTRATION NUMBER: NCT03737968.