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Toward personalized lymphoma immunotherapy: Identification of common driver mutations recognized by patient CD8+ T cells.

Clin Cancer Res.. 2016-05; 
Nielsen JS, Sedgwick CG, Shahid A, Zong Z, Brumme ZL, Yu S, Liu L, Kroeger DR, Treon SP, Connors JM, Gascoyne RD, Berry BR, Marra MA, Morin RD, Macpherson N, Nelson BH1.
Products/Services Used Details Operation
Peptide Synthesis ... IC50 binding score <1000 nM (and wild type counterparts as required) were synthesized and purified commercially (ThinkPeptides and Genscript), reconstituted in 80% DMSO, and stored at - 80°C. In vitro T cell priming ... Sanger sequencing (Genscript). ... Get A Quote

摘要

PURPOSE: A fundamental challenge in the era of next-generation sequencing (NGS) is to design effective treatments tailored to the mutational profiles of tumors. Many newly discovered cancer mutations are difficult to target pharmacologically; however, T-cell-based therapies may provide a valuable alternative owing to the exquisite sensitivity and specificity of antigen recognition. To explore this concept, we assessed the immunogenicity of a panel of genes that are common sites of driver mutations in follicular lymphoma, an immunologically sensitive yet currently incurable disease. EXPERIMENTAL DESIGN: Exon capture and NGS were used to interrogate tumor samples from 53 patients with follicular lymphoma for mu... More

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