Prevalent and Diverse Intratumoral Oncoprotein-Specific CD8 T Cells Within Polyomavirus-Driven Merkel Cell Carcinomas

Overview

Journal Cancer Immunol Res

Specialties Allergy & Immunology
Oncology

Date 2020 Mar 18

PMID 32179557

Citations 26

Authors

Lichen Jing

Mariliis Ott

Candice D Church

Rima M Kulikauskas

Dafina Ibrani

Jayasri G Iyer

Olga K Afanasiev

Aric Colunga

Maclean M Cook

Hong Xie

Alexander L Greninger

Kelly G Paulson

Aude G Chapuis

Shailender Bhatia

Paul Nghiem

David M Koelle

Affiliations

Soon will be listed here.

Abstract

Merkel cell carcinoma (MCC) is often caused by persistent expression of Merkel cell polyomavirus (MCPyV) T-antigen (T-Ag). These non-self proteins comprise about 400 amino acids (AA). Clinical responses to immune checkpoint inhibitors, seen in about half of patients, may relate to T-Ag-specific T cells. Strategies to increase CD8 T-cell number, breadth, or function could augment checkpoint inhibition, but vaccines to augment immunity must avoid delivery of oncogenic T-antigen domains. We probed MCC tumor-infiltrating lymphocytes (TIL) with an artificial antigen-presenting cell (aAPC) system and confirmed T-Ag recognition with synthetic peptides, HLA-peptide tetramers, and dendritic cells (DC). TILs from 9 of 12 (75%) subjects contained CD8 T cells recognizing 1-8 MCPyV epitopes per person. Analysis of 16 MCPyV CD8 TIL epitopes and prior TIL data indicated that 97% of patients with MCPyV MCC had HLA alleles with the genetic potential that restrict CD8 T-cell responses to MCPyV T-Ag. The LT AA 70-110 region was epitope rich, whereas the oncogenic domains of T-Ag were not commonly recognized. Specific recognition of T-Ag-expressing DCs was documented. Recovery of MCPyV oncoprotein-specific CD8 TILs from most tumors indicated that antigen indifference was unlikely to be a major cause of checkpoint inhibition failure. The myriad of epitopes restricted by diverse HLA alleles indicates that vaccination can be a rational component of immunotherapy if tumor immune suppression can be overcome, and the oncogenic regions of T-Ag can be modified without impacting immunogenicity.

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