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Detection of neoantigen-specific T cells following a personalized vaccine in a patient with glioblastoma.

Oncoimmunology. 2019-01; 
JohannsTanner M,MillerChristopher A,LiuConnor J,PerrinRichard J,BenderDiane,KobayashiDale K,CampianJian L,ChicoineMichael R,DaceyRalph G,HuangJiayi,FritschEdward F,GillandersWilliam E,ArtyomovMaxim N,MardisElaine R,SchreiberRobert D,DunnGav
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Peptide Synthesis Approximately 100,000 double-negative autologous PBMC were incubated on pre-coated human IFN-γ ELISPOT plates with 10 μM of indicated peptide (GenScript, Piscataway, NJ) plus ~400,000 CD8+ or CD4+ PBMC, or ~20,000 CD8+ or CD4+ TIL for 18–20 hours at 37°C. Get A Quote

摘要

Neoantigens represent promising targets for personalized cancer vaccine strategies. However, the feasibility of this approach in lower mutational burden tumors like glioblastoma (GBM) remains unknown. We have previously reported the use of an immunogenomics pipeline to identify candidate neoantigens in preclinical models of GBM. Here, we report the application of the same immunogenomics pipeline to identify candidate neoantigens and guide screening for neoantigen-specific T cell responses in a patient with GBM treated with a personalized synthetic long peptide vaccine following autologous tumor lysate DC vaccination. Following vaccination, reactivity to three HLA class I- and five HLA class II-restricted ... More

关键词

Neoantigen,clonal evolution,glioblastoma,immunogenomics,personalized vac
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