DNA Vaccines Targeting Novel Cancer-Associated Antigens Frequently Expressed in Head and Neck Cancer Enhance the Efficacy of Checkpoint Inhibitor.

Chuan Wang,Rosnah Binti Zain,Natasha Zulaziz,Ruhcha V Sutavani,Shin Hin Lau,Chai Phei Gan,Mannil Thomas Abraham,San Jiun Chai,Sok Ching Cheong,Gareth J Thomas,Zainal Ariff Abdul Rahman,Thomas George Kallarakkal,Christian H Ottensmeier,Natalia Savelyeva,Nur Syafinaz Zainal ,Bryan Kit Weng Lye ,S.m Ismail ,Kein Seong Mun ,Emma V King ,James Dickie ,Ka Keat Lim

doi:10.3389/fimmu.2021.763086

Abstract

HPV-independent head and neck squamous cell carcinoma (HNSCC) is a common cancer globally. The overall response rate to anti-PD1 checkpoint inhibitors (CPIs) in HNSCC is ~16%. One major factor influencing the effectiveness of CPI is the level of tumor infiltrating T cells (TILs). Converting TILlow tumors to TILhigh tumors is thus critical to improve clinical outcome. Here we describe a novel DNA vaccines to facilitate the T-cell infiltration and control tumor growth. We evaluated the expression of target antigens and their respective immunogenicity in HNSCC patients. The efficacy of DNA vaccines targeting two novel antigens were evaluated with or without CPI using a syngeneic model. Most HNSCC patients (43/44) co-expressed MAGED4B and FJX1 and their respective tetramer-specific T cells were in the range of 0.06-0.12%. In a preclinical model, antigen-specific T cells were induced by DNA vaccines and increased T cell infiltration into the tumor, but not MDSC or regulatory T cells. The vaccines inhibited tumor growth and improved the outcome alone and upon combination with anti-PD1 and resulted in tumor clearance in approximately 75% of mice. Pre-existence of MAGED4B and FJX1-reactive T cells in HNSCC patients suggests that these widely expressed antigens are highly immunogenic and could be further expanded by vaccination. The DNA vaccines targeting these antigens induced robust T cell responses and with the anti-PD1 antibody conferring excellent tumor control. This opens up an opportunity for combination immunotherapy that might benefit a wider population of HNSCC patients in an antigen-specific manner.

Highlights

HNSCC is the sixth most common cancer in the world and is more prevalent in South East Asia where it is the second most common malignancy [1]
Using TCGA-HNSC project data, we demonstrated that both MAGED4B and FJX1 gene expression levels in the HPV negative (n=415) and HPV positive (n=72) tumour tissue samples were significantly higher than levels in adjacent normal tissues (n=44, Figure 1A)
Most well-characterized cancer testis antigens (CTA) are not expressed in a large proportion of head and neck cancer [49]

Summary

Introduction

HNSCC is the sixth most common cancer in the world and is more prevalent in South East Asia where it is the second most common malignancy [1]. TILlow tumors, including most HPVneg HNSCC, are commonly categorized as ‘immune desert’ (absent T cells) or ‘immune excluded’ (excluded T cells) [13, 16, 17]. This emphasizes the urgent need of novel immunotherapies that can work in these patients. One such intervention is to use cancer vaccines to induce or expand specific T cell responses against cancer

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