| Literature DB >> 33016924 |
Gal Cafri1,2, Jared J Gartner1, Tal Zaks3, Kristen Hopson3, Noam Levin1, Biman C Paria1, Maria R Parkhurst1, Rami Yossef1, Frank J Lowery1, Mohammad S Jafferji1, Todd D Prickett1, Stephanie L Goff1, Christine T McGowan1, Samantha Seitter1, Mackenzie L Shindorf1, Anup Parikh1, Praveen D Chatani1, Paul F Robbins1, Steven A Rosenberg1.
Abstract
BACKGROUNDTherapeutic vaccinations against cancer have mainly targeted differentiation antigens, cancer-testis antigens, and overexpressed antigens and have thus far resulted in little clinical benefit. Studies conducted by multiple groups have demonstrated that T cells recognizing neoantigens are present in most cancers and offer a specific and highly immunogenic target for personalized vaccination.METHODSWe recently developed a process using tumor-infiltrating lymphocytes to identify the specific immunogenic mutations expressed in patients' tumors. Here, validated, defined neoantigens, predicted neoepitopes, and mutations of driver genes were concatenated into a single mRNA construct to vaccinate patients with metastatic gastrointestinal cancer.RESULTSThe vaccine was safe and elicited mutation-specific T cell responses against predicted neoepitopes not detected before vaccination. Furthermore, we were able to isolate and verify T cell receptors targeting KRASG12D mutation. We observed no objective clinical responses in the 4 patients treated in this trial.CONCLUSIONThis vaccine was safe, and potential future combination of such vaccines with checkpoint inhibitors or adoptive T cell therapy should be evaluated for possible clinical benefit in patients with common epithelial cancers.TRIAL REGISTRATIONPhase I/II protocol (NCT03480152) was approved by the IRB committee of the NIH and the FDA.FUNDINGCenter for Clinical Research, NCI, NIH.Entities:
Keywords: Cancer immunotherapy; Oncology; Vaccines
Year: 2020 PMID: 33016924 PMCID: PMC7598064 DOI: 10.1172/JCI134915
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808