Mutational and putative neoantigen load predict clinical benefit of adoptive T cell therapy in melanoma

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Martin Lauss
Marco Donia
Katja Harbst
Rikke Andersen
Shamik Mitra
Frida Rosengren
Maryem Salim
Johan Vallon-Christersson
Therese Törngren
Anders Kvist
Markus Ringnér
Inge Marie Svane
Göran Jönsson
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[1] Lund University,Division of Oncology and Pathology, Department of Clinical Sciences Lund, Faculty of Medicine
[2] Department of Hematology,Center for Cancer Immune Therapy
[3] Copenhagen University Hospital Herlev,Department of Oncology
[4] Lund University,Department of Biology, National Bioinformatics Infrastructure Sweden, Science for Life Laboratory
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Adoptive T-cell therapy (ACT) is a highly intensive immunotherapy regime that has yielded remarkable response rates and many durable responses in clinical trials in melanoma; however, 50–60% of the patients have no clinical benefit. Here, we searched for predictive biomarkers to ACT in melanoma. Whole exome- and transcriptome sequencing and neoantigen prediction were applied to pre-treatment samples from 27 patients recruited to a clinical phase I/II trial of ACT in stage IV melanoma. All patients had previously progressed on other immunotherapies. We report that clinical benefit is associated with significantly higher predicted neoantigen load. High mutation and predicted neoantigen load are significantly associated with improved progression-free and overall survival. Further, clinical benefit is associated with the expression of immune activation signatures including a high MHC-I antigen processing and presentation score. These results improve our understanding of mechanisms behind clinical benefit of ACT in melanoma.
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