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CAR-engineered lymphocyte persistence is governed by a FAS ligand/FAS auto-regulatory circuit

biorxiv. 2024-03; 
Fei Yi, Tal Cohen, Natalie Zimmerman, Friederike Dündar, Paul Zumbo, Razan Eltilib, Erica J Brophy, Hannah Arkin, Judith Feucht, Michael V Gormally, Christopher S Hackett, Korbinian N Kropp, Inaki Etxeberria, Smita S Chandran, Jae H Park, Katharine C Hsu, Michel Sadelain, Doron Betel, Christopher A Klebanoff
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Gene Synthesis … motifs and synthesized by Genscript. The synthesized genes … Genscript). Similarly, NLS-mCherry and NLS-GFP sequences were synthesized and cloned into an SFG vector by Genscript Get A Quote

摘要

Chimeric antigen receptor (CAR)-engineered T and NK cells can cause durable remission of B-cell malignancies; however, limited persistence restrains the full potential of these therapies in many patients. The FAS ligand (FAS-L)/FAS pathway governs naturally-occurring lymphocyte homeostasis, yet knowledge of which cells express FAS-L in patients and whether these sources compromise CAR persistence remains incomplete. Here, we constructed a single-cell atlas of diverse cancer types to identify cellular subsets expressing , the gene encoding FAS-L. We discovered that is limited primarily to endogenous T cells, NK cells, and CAR-T cells while tumor and stromal cells express minimal . To establish whether CAR-T/NK ... More

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