The common HLA class I-restricted tumor-infiltrating T cell response in HPV16-induced cancer

被引:0
|
作者
Saskia J. Santegoets
Marij J. P. Welters
Deborah S. Schrikkema
Manon R. Freriks
Hanna Kok
Bianca Weissbrich
Anouk van den Branden
Carsten Linnemann
Ton N. Schumacher
Sabina Adhikary
Gavin Bendle
Sjoerd H. van der Burg
机构
[1] Leiden University Medical Center,Department of Medical Oncology, Oncode Institute
[2] Kite,Division of Molecular Oncology and Immunology, Oncode Institute
[3] a Gilead Company,Department of Hematology
[4] The Netherlands Cancer Institute,undefined
[5] Leiden University Medical Center,undefined
[6] Kite,undefined
[7] a Gilead Company,undefined
来源
Cancer Immunology, Immunotherapy | 2023年 / 72卷
关键词
HPV16; TCR gene transfer; TIL;
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学科分类号
摘要
Immunotherapies targeting truly tumor-specific targets focus on the expansion and activation of T cells against neoantigens or oncogenic viruses. One target is the human papilloma virus type 16 (HPV16), responsible for several anogenital cancers and oropharyngeal carcinomas. Spontaneous and vaccine-induced HPV-specific T cells have been associated with better clinical outcome. However, the epitopes and restriction elements to which these T cells respond remained elusive. To identify CD8+ T cell epitopes in cultures of tumor infiltrating lymphocytes, we here used multimers and/or a functional screening platform exploiting single HLA class I allele-engineered antigen presenting cells. This resulted in the detection of 20 CD8+ T cell responses to 11 different endogenously processed HLA-peptide combinations within 12 HPV16-induced tumors. Specific HLA-peptide combinations dominated the response in patients expressing these HLA alleles. T cell receptors (TCRs) reactive to seven different HLA class I-restricted peptides could be isolated and analysis revealed tumor reactivity for five of the six TCRs analyzed. The tumor reactive TCRs to these dominant HLA class I peptide combinations can potentially be used to engineer tumor-specific T cells for adoptive cell transfer approaches to treat HPV16-induced cancers.
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页码:1553 / 1565
页数:12
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