CD4+ T cell calibration of antigen-presenting cells optimizes antiviral CD8+ T cell immunity

被引:9
|
作者
Gressier, Elise [1 ]
Schulte-Schrepping, Jonas [2 ,3 ]
Petrov, Lev [4 ,5 ]
Brumhard, Sophia [6 ]
Stubbemann, Paula [6 ]
Hiller, Anna [6 ]
Obermayer, Benedikt [7 ]
Spitzer, Jasper [8 ]
Kostevc, Tomislav [4 ,5 ]
Whitney, Paul G. [1 ]
Bachem, Annabell [1 ]
Odainic, Alexandru [1 ,8 ]
van de Sandt, Carolien [1 ]
Nguyen, Thi H. O. [1 ]
Ashhurst, Thomas [9 ,10 ]
Wilson, Kayla [1 ]
Oates, Clare V. L. [1 ]
Gearing, Linden. J. [11 ,12 ]
Meischel, Tina [1 ]
Hochheiser, Katharina [1 ]
Greyer, Marie [1 ]
Clarke, Michele [1 ]
Kreutzenbeck, Maike [8 ]
Gabriel, Sarah S. [1 ]
Kastenmueller, Wolfgang [13 ]
Kurts, Christian [14 ]
Londrigan, Sarah L. [1 ]
Kallies, Axel [1 ]
Kedzierska, Katherine [1 ]
Hertzog, Paul J. [11 ,12 ]
Latz, Eicke [8 ]
Chen, Yu-Chen E. [15 ]
Radford, Kristen J. [15 ]
Chopin, Michael [16 ]
Schroeder, Jan [1 ]
Kurth, Florian [6 ]
Gebhardt, Thomas [1 ]
Sander, Leif E. [6 ]
Sawitzki, Birgit [4 ,5 ]
Schultze, Joachim L. [2 ,3 ,17 ,18 ]
Schmidt, Susanne V. [8 ]
Bedoui, Sammy [1 ,14 ]
机构
[1] Univ Melbourne, Dept Microbiol & Immunol, Doherty Inst Infect & Immun, Melbourne, Vic, Australia
[2] Univ Bonn, Life & Med Sci LIMES Inst, Bonn, Germany
[3] DZNE, Syst Med, Bonn, Germany
[4] Berlin Inst Hlth, Translat Immunol, Berlin, Germany
[5] Charite, Berlin, Germany
[6] Charite Univ Med Berlin, Infect Dis & Resp Med, Berlin, Germany
[7] Charite Univ Med Berlin, Berlin Inst Hlth, Core Unit Bioinformat, Berlin, Germany
[8] Univ Bonn, Inst Innate Immun, Bonn, Germany
[9] Centenary Inst, Charles Perkins Ctr, Sydney Cytometry Core Res Facil, Sydney, NSW, Australia
[10] Univ Sydney, Sydney, NSW, Australia
[11] Hudson Inst Med Res, Ctr Innate Immun & Infect Dis, Clayton, Vic, Australia
[12] Monash Univ, Dept Mol & Translat Sci, Clayton, Vic, Australia
[13] Julius Maximilians Univ Wurzburg, Wurzburg Inst Syst Immunol, Max Planck Res Grp, Wurzburg, Germany
[14] Univ Bonn, Inst Expt Immunol, Bonn, Germany
[15] Univ Queensland, Mater Res Inst, Brisbane, Qld, Australia
[16] Monash Univ, Biomed Discovery Inst, Dept Biochem, Clayton, Vic, Australia
[17] DZNE, PRECISE Platform Single Cell Genom & Epigen, Bonn, Germany
[18] Univ Bonn, Bonn, Germany
基金
欧盟地平线“2020”; 英国医学研究理事会;
关键词
DIFFERENTIATION; ACTIVATION; SARS-COV-2; RESPONSES; COVID-19; EFFECTOR; REQUIRES; MILD;
D O I
10.1038/s41590-023-01517-x
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Bedoui and colleagues describe a sequential process of integration of innate and CD40-delivered signals in APCs, which optimizes their capacity to drive antiviral CD8(+) T cell responses. 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-alpha/interferon-beta (IFN alpha/beta)-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 IFN alpha/beta 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.
引用
收藏
页码:979 / +
页数:26
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