| Literature DB >> 33796222 |
Charles R Schutt1,2, Hua Sun1,3,2, Jaya Sarin Pradhan4, Yvonne Saenger5, Jessica Ley1, Douglas Adkins1,6, Matthew Ingham5, Li Ding1,3,7,6, Brian A Van Tine1,8,6.
Abstract
Head and neck cell squamous-cell carcinomas (HNSCC) are a group of common cancers typically associated with tobacco use and human papilloma virus infection. Up to half of all cases will suffer a recurrence after primary treatment. As such, new therapies are needed, including therapies which promote the anti-tumor immune response. Prior work has characterized changes in the mutation burden between primary and recurrent tumors; however, little work has characterized the changes in neoantigen evolution. We characterized genomic and neoantigen changes between 23 paired primary and recurrent HNSCC tumors. Twenty-three biopsies from patients originally diagnosed with locally advanced disease were identified from the Washington University tumor bank. Whole exosome sequencing, RNA-seq, and immunohistochemistry was performed on the primary and recurrent tumors. Within these tumors, we identified 6 genes which have predicted neoantigens in 4 or more patients. Interestingly, patients with neoantigens in these shared genes had increased CD3+ CD8+ T cell infiltration and duration of survival with disease. Within HNSCC tumors examined here, there are neoantigens in shared genes by a subset of patients. The presence of neoantigens in these shared genes may promote an anti-tumor immune response which controls tumor progression. Copyright:Entities:
Keywords: head and neck squamous cell carcinoma; immune cell infiltration; mutational evolution; neoantigens; tumor relapse
Year: 2021 PMID: 33796222 PMCID: PMC7984826 DOI: 10.18632/oncotarget.27907
Source DB: PubMed Journal: Oncotarget ISSN: 1949-2553