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Radiotherapy and Cisplatin Increase Immunotherapy Efficacy by Enabling Local and Systemic Intratumoral T-cell Activity.

Paula Kroon ,
Elselien Frijlink ,
Victoria Iglesias-Guimarais ,
Andriy Volkov ,
Marit M van Buuren ,
Ton N Schumacher ,
Marcel Verheij ,
Jannie Borst ,
Inge Verbrugge

Abstract

To increase cancer immunotherapy success, PD-1 blockade must be combined with rationally selected treatments. Here, we examined, in a poorly immunogenic mouse breast cancer model, the potential of antibody-based immunomodulation and conventional anticancer treatments to collaborate with anti-PD-1 treatment. One requirement to improve anti-PD-1-mediated tumor control was to promote tumor-specific cytotoxic T-cell (CTL) priming, which was achieved by stimulating the CD137 costimulatory receptor. A second requirement was to overrule PD-1-unrelated mechanisms of CTL suppression in the tumor microenvironment (TME). This was achieved by radiotherapy and cisplatin treatment. In the context of CD137/PD-1-targeting immunotherapy, radiotherapy allowed for tumor elimination by altering the TME, rather than intrinsic CTL functionality. Combining this radioimmunotherapy regimen with low-dose cisplatin improved CTL-dependent regression of a contralateral tumor outside the radiation field. Thus, systemic tumor control may be achieved by combining immunotherapy protocols that promote T-cell priming with (chemo)radiation protocols that permit CTL activity in both the irradiated tumor and (occult) metastases.

More about this publication

Cancer immunology research

Volume 7
Issue nr. 4
Pages 670-682
Publication date 01-04-2019

Full text links

Publisher website (DOI) 10.1158/2326-6066.CIR-18-0654
Europe PubMed Central 30782666
Pubmed 30782666

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