Phase I trial of viral vector based personalized vaccination elicits robust neoantigen specific antitumor T cell responses.

Anna Morena D'Alise Guido Leoni Gabriella Cotugno Loredana Siani Rosa Vitale Valentino Ruzza Irene Garzia Laura Antonucci Elisa Micarelli Veronica Venafra Sven Gogov Alessia Capone Sarah Runswick Juan Martín-Liberal Emiliano Calvo Victor Moreno Stefan N Symeonides Elisa Scarselli Oliver Bechter

Published in: Clinical cancer research : an official journal of the American Association for Cancer Research (2024)

These findings indicate the ability of NOUS-PEV to amplify and broaden the repertoire of tumor reactive T cells to empower a diverse, potent and durable antitumor immune response. Finally, a gene signature indicative for reduced presence of activated T cells together with very poor expression of the antigen processing machinery (APM) genes has been identified in pre-treatment biopsies as a potential biomarker of resistance to the treatment.

Keyphrases

immune response
genome wide
poor prognosis
clinical trial
sars cov
randomized controlled trial
gene expression
dna methylation
dendritic cells
replacement therapy
open label
genome wide analysis
double blind
high throughput sequencing