Multimodal stimulation screens reveal unique and shared genes limiting T cell fitness
Publication date
2024-04-08
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Abstract
Genes limiting T cell antitumor activity may serve as therapeutic targets. It has not been systematically studied whether there are regulators that uniquely or broadly contribute to T cell fitness. We perform genome-scale CRISPR-Cas9 knockout screens in primary CD8 T cells to uncover genes negatively impacting fitness upon three modes of stimulation: (1) intense, triggering activation-induced cell death (AICD); (2) acute, triggering expansion; (3) chronic, causing dysfunction. Besides established regulators, we uncover genes controlling T cell fitness either specifically or commonly upon differential stimulation. Dap5 ablation, ranking highly in all three screens, increases translation while enhancing tumor killing. Loss of Icam1-mediated homotypic T cell clustering amplifies cell expansion and effector functions after both acute and intense stimulation. Lastly, Ctbp1 inactivation induces functional T cell persistence exclusively upon chronic stimulation. Our results functionally annotate fitness regulators based on their unique or shared contribution to traits limiting T cell antitumor activity.
Keywords
activation-induced cell death, cancer immunotherapy, CRISPR-Cas9 screen, Ctbp1, Dap5, dysfunction, effector function, exhaustion, Icam1, T cells, Oncology, Cancer Research, SDG 3 - Good Health and Well-being
Citation
Lin, C P, Levy, P L, Alflen, A, Apriamashvili, G, Ligtenberg, M A, Vredevoogd, D W, Bleijerveld, O B, Alkan, F, Malka, Y, Hoekman, L, Markovits, E, George, A, Traets, J J H, Krijgsman, O, van Vliet, A, Poźniak, J, Pulido-Vicuña, C A, de Bruijn, B, van Hal-van Veen, S E, Boshuizen, J, van der Helm, P W, Díaz-Gómez, J, Warda, H, Behrens, L M, Mardesic, P, Dehni, B, Visser, N L, Marine, J C, Markel, G, Faller, W J, Altelaar, M, Agami, R, Besser, M J & Peeper, D S 2024, 'Multimodal stimulation screens reveal unique and shared genes limiting T cell fitness', Cancer Cell, vol. 42, no. 4, e10, pp. 623-645. https://doi.org/10.1016/j.ccell.2024.02.016