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Antigen-specific TIL therapy for melanoma: A flexible platform for personalized cancer immunotherapy.

Sander Kelderman ,
Bianca Heemskerk ,
Lorenzo Fanchi ,
Daisy Philips ,
Mireille Toebes ,
Pia Kvistborg ,
Marit M van Buuren ,
Nienke van Rooij ,
Samira Michels ,
Lothar Germeroth ,
John B A G Haanen ,
N M Schumacher

Abstract

Tumor infiltrating lymphocyte (TIL) therapy has shown objective clinical response rates of 50% in stage IV melanoma patients in a number of clinical trials. Nevertheless, the majority of patients progress either directly upon therapy or after an initial period of tumor control. Recent data have shown that most TIL products that are used for therapy contain only low frequencies of T cells reactive against known melanoma-associated epitopes. Because of this, the development of a technology to create T-cell products that are enriched for reactivity against defined melanoma-associated antigens would seem valuable, both to evaluate the tumoricidal potential of T cells directed against different antigen classes and to potentially increase response rates. Here, we developed and validated a conditional MHC streptamer-based platform for the creation of TIL products with defined antigen reactivities. We have used this platform to successfully enrich both high-frequency (≥1%) and low-frequency (<1%) tumor-specific CD8(+) T-cell populations, and thereby created T-cell products with enhanced tumor recognition potential. Collectively, these data demonstrate that selection of antigen-specific T-cell populations can be used to create defined T-cell products for clinical use. This strategy thus forms a highly flexible platform for the development of antigen-specific cell products for personalized cancer immunotherapy.

More about this publication

European journal of immunology

Volume 46
Issue nr. 6
Pages 1351-60
Publication date 01-06-2016

Full text links

Publisher website (DOI) 10.1002/eji.201545849
Europe PubMed Central 27005018
Pubmed 27005018

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