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Mis-splicing-derived neoantigens and cognate TCRs in splicing factor mutant leukemias

Cell. 2025-04; 
Won Jun Kim, Edie I Crosse, Emma De Neef, Inaki Etxeberria, Erich Y Sabio, Eric Wang, Jan Philipp Bewersdorf, Kuan-Ting Lin, Sydney X Lu, Andrea Belleville, Nina Fox, Cynthia Castro, Pu Zhang, Takeshi Fujino, Jennifer Lewis, Jahan Rahman, Beatrice Zhang, Jacob H Winick, Alexander M Lewis, Robert F Stanley, Susan DeWolf, Brigita Meškauskaitė Urben, Meril Takizawa, Tobias Krause, Henrik Molina, Ronan Chaligne, Priya Koppikar, Jeffrey Molldrem, Mathieu Gigoux, Taha Merghoub, Anthony Daniyan, Smita S Chandran, Benjamin D Greenbaum, Christopher A Klebanoff, Robert K Bradley, Omar Abdel-Wahab Memorial Sloan Kettering Cancer Center
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Gene Synthesis NLS-eGFP and NLS-mCherry sequences were synthesized and cloned into pMSGV-1 RV plasmid by Genscript. Full-length and mis-spliced isoform cDNA sequences of CLK3, RHOT2, and c16orf70 were cloned into pcDNA3.1+ vector by Genscript.>98% purity peptides were synthesized by Genscript, with standard removal of trifluoroacetic acid (TFA) and replacement with chloride.A set of 9-mer peptides, where each of the amino acid residues of the CLK3 neoantigen (RLWGTWVKA) was substituted with alanine (or glycine for the amino acid #9), were synthesized by Genscript.For TCR2, five potential off-target peptides predicted by ScanProsite were synthesized by Genscript and tested for CLK3 TCR-T cell activation as described above. Get A Quote

摘要

Mutations in RNA splicing factors are prevalent across cancers and generate recurrently mis-spliced mRNA isoforms. Here, we identified a series of bona fide neoantigens translated from highly stereotyped splicing alterations promoted by neomorphic, leukemia-associated somatic splicing machinery mutations. We utilized feature-barcoded peptide-major histocompatibility complex (MHC) dextramers to isolate neoantigen-reactive T cell receptors (TCRs) from healthy donors, patients with active myeloid malignancy, and following curative allogeneic stem cell transplant. Neoantigen-reactive CD8+ T cells were present in the blood of patients with active cancer and had a distinct phenotype from virus-reactive T cells with e... More

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