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Molecular Recalibration of PD-1+ Antigen-Specific T Cells from Blood and Liver.

Mol. Ther.. 2018; 
OtanoItziar,EscorsDavid,SchurichAnna,SinghHarsimran,RobertsonFrancis,DavidsonBrian R,FusaiGiuseppe,VargasFrederick A,TanZhi M D,AwJia Y J,HansiNavjyot,KennedyPatrick T F,XueShao-An,StaussHans J,BertolettiAntonio,PavesiAndrea,MainiMa
Products/Services Used Details Operation
Gene Synthesis LV-shCTR was generated, replacing the shPD-1 sequence for a control shRNA (50 -CCTAAGGTTAAGTCGCCCTCG-30 ), and mCherry constructs were generated by GenScript (USA). Get A Quote

摘要

Checkpoint inhibitors and adoptive cell therapy provide promising options for treating solid cancers such as HBV-related HCC, but they have limitations. We tested the potential to combine advantages of each approach, genetically reprogramming T cells specific for viral tumor antigens to overcome exhaustion by down-modulating the co-inhibitory receptor PD-1. We developed a novel lentiviral transduction protocol to achieve preferential targeting of endogenous or TCR-redirected, antigen-specific CD8 T cells for shRNA knockdown of PD-1 and tested functional consequences for antitumor immunity. Antigen-specific and intrahepatic CD8 T cells transduced with lentiviral (LV)-shPD-1 consistently had a marked red... More

关键词

3D models,HBV,HCC,PD-1,TCR-redirected T cells,anti-tumor immunity,cell therapy,checkpoints,genetic modification,immunotherapy,shRNA knock