细胞毒性T细胞
T细胞
生物
抗原提呈细胞
获得性免疫系统
免疫学
干扰素
CD8型
CD40
白细胞介素2受体
抗原呈递
细胞生物学
效应器
先天免疫系统
免疫
抗原
免疫系统
体外
遗传学
作者
Elise Gressier,Jonas Schulte-Schrepping,L. A. Petrov,Sophia Brumhard,Paula Stubbemann,Anna Luisa Hiller,Benedikt Obermayer,Jasper Spitzer,Tomislav Kostevc,Paul G. Whitney,Annabell Bachem,Alexandru Odainic,Carolien E. van de Sandt,Thi H. O. Nguyen,Thomas M. Ashhurst,Kayla R. Wilson,Clare V. Oates,Linden J. Gearing,Tina Meischel,Katharina Hochheiser
标识
DOI:10.1038/s41590-023-01517-x
摘要
Antiviral CD8+ T cell immunity depends on the integration of various contextual cues, but how antigen-presenting cells (APCs) consolidate these signals for decoding by T cells remains unclear. Here, we describe gradual interferon-α/interferon-β (IFNα/β)-induced transcriptional adaptations that endow APCs with the capacity to rapidly activate the transcriptional regulators p65, IRF1 and FOS after CD4+ T cell-mediated CD40 stimulation. While these responses operate through broadly used signaling components, they induce a unique set of co-stimulatory molecules and soluble mediators that cannot be elicited by IFNα/β or CD40 alone. These responses are critical for the acquisition of antiviral CD8+ T cell effector function, and their activity in APCs from individuals infected with severe acute respiratory syndrome coronavirus 2 correlates with milder disease. These observations uncover a sequential integration process whereby APCs rely on CD4+ T cells to select the innate circuits that guide antiviral CD8+ T cell responses.
科研通智能强力驱动
Strongly Powered by AbleSci AI