CD5 signalosome coordinates antagonist TCR signals to control the generation of Treg cells induced by foreign antigens.
Gaëtan BlaizeHélène Daniels-TreffandierMeryem AloulouNelly RouquiéCui YangMarlène MarcellinMylène GadorMehdi BenamarMariette F DucatezKi-Duk SongOdile Burlet-SchiltzAbdelhadi SaoudiPaul E LoveNicolas FazilleauAnne Gonzalez de PeredoRenaud LesournePublished in: Proceedings of the National Academy of Sciences of the United States of America (2020)
CD5 is characterized as an inhibitory coreceptor with an important regulatory role during T cell development. The molecular mechanism by which CD5 operates has been puzzling and its function in mature T cells suggests promoting rather than repressing effects on immune responses. Here, we combined quantitative mass spectrometry and genetic studies to analyze the components and the activity of the CD5 signaling machinery in primary T cells. We found that T cell receptor (TCR) engagement induces the selective phosphorylation of CD5 tyrosine 429, which serves as a docking site for proteins with adaptor functions (c-Cbl, CIN85, CRKL), connecting CD5 to positive (PI3K) and negative (UBASH3A, SHIP1) regulators of TCR signaling. c-CBL acts as a coordinator in this complex enabling CD5 to synchronize positive and negative feedbacks on TCR signaling through the other components. Disruption of CD5 signalosome in mutant mice reveals that it modulates TCR signal outputs to selectively repress the transactivation of Foxp3 and limit the inopportune induction of peripherally induced regulatory T cells during immune responses against foreign antigen. Our findings bring insights into the paradigm of coreceptor signaling, suggesting that, in addition to providing dualistic enhancing or dampening inputs, coreceptors can engage concomitant stimulatory and inhibitory signaling events, which act together to promote specific functional outcomes.
Keyphrases
- regulatory t cells
- immune response
- dendritic cells
- mass spectrometry
- nk cells
- high resolution
- transcription factor
- gene expression
- cell proliferation
- cell death
- inflammatory response
- small molecule
- liquid chromatography
- high glucose
- protein protein
- simultaneous determination
- capillary electrophoresis
- tandem mass spectrometry
- solid phase extraction