| Literature DB >> 36175679 |
Ye Li1,2, Rafet Basar1, Guohui Wang1, Enli Liu1, Judy S Moyes1, Li Li1, Lucila N Kerbauy1,3,4, Nadima Uprety1, Mohsen Fathi5, Ali Rezvan5, Pinaki P Banerjee1, Luis Muniz-Feliciano1, Tamara J Laskowski1, Emily Ensley1, May Daher1, Mayra Shanley1, Mayela Mendt1, Sunil Acharya1, Bin Liu1, Alexander Biederstädt1,6, Hind Rafei1, Xingliang Guo1, Luciana Melo Garcia1, Paul Lin1, Sonny Ang1, David Marin1, Ken Chen7, Laura Bover8,9, Richard E Champlin1, Navin Varadarajan5, Elizabeth J Shpall1, Katayoun Rezvani10.
Abstract
Trogocytosis is an active process that transfers surface material from targeted to effector cells. Using multiple in vivo tumor models and clinical data, we report that chimeric antigen receptor (CAR) activation in natural killer (NK) cells promoted transfer of the CAR cognate antigen from tumor to NK cells, resulting in (1) lower tumor antigen density, thus impairing the ability of CAR-NK cells to engage with their target, and (2) induced self-recognition and continuous CAR-mediated engagement, resulting in fratricide of trogocytic antigen-expressing NK cells (NKTROG+) and NK cell hyporesponsiveness. This phenomenon could be offset by a dual-CAR system incorporating both an activating CAR against the cognate tumor antigen and an NK self-recognizing inhibitory CAR that transferred a 'don't kill me' signal to NK cells upon engagement with their TROG+ siblings. This system prevented trogocytic antigen-mediated fratricide, while sparing activating CAR signaling against the tumor antigen, and resulted in enhanced CAR-NK cell activity.Entities:
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Year: 2022 PMID: 36175679 DOI: 10.1038/s41591-022-02003-x
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 87.241