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Literature DB >> 32412411

Stimulation strength controls the rate of initiation but not the molecular organisation of TCR-induced signalling.

John C Marioni^1,2,3, Gillian M Griffiths⁴, Arianne C Richard^4,1, Claire Y Ma⁴.

Abstract

Millions of naïve T cells with different TCRs may interact with a peptide-MHC ligand, but very few will activate. Remarkably, this fine control is orchestrated using a limited set of intracellular machinery. It remains unclear whether changes in stimulation strength alter the programme of signalling events leading to T cell activation. Using mass cytometry to simultaneously measure multiple signalling pathways during activation of murine CD8+ T cells, we found a programme of distal signalling events that is shared, regardless of the strength of TCR stimulation. Moreover, the relationship between transcription of early response genes Nr4a1 and Irf8 and activation of the ribosomal protein S6 is also conserved across stimuli. Instead, we found that stimulation strength dictates the rate with which cells initiate signalling through this network. These data suggest that TCR-induced signalling results in a coordinated activation program, modulated in rate but not organization by stimulation strength.

Entities: Chemical

Keywords: CD8 T cells; T cell receptor; computational biology; immunology; inflammation; mass cytometry; mouse; signalling; systems biology

Mesh：

Substances：

Year: 2020 PMID： 32412411 PMCID： PMC7308083 DOI： 10.7554/eLife.53948

Source DB: PubMed Journal: Elife ISSN： 2050-084X Impact factor: 8.140

105 in total

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Stimulation strength controls the rate of initiation but not the molecular organisation of TCR-induced signalling.

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Review 6. Signal transduction via the T cell antigen receptor in naïve and effector/memory T cells.

7. Accumulation of dynamic catch bonds between TCR and agonist peptide-MHC triggers T cell signaling.

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Review 4. CD28 Costimulation: From Mechanism to Therapy.

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Review 1. Divide and Conquer: Phenotypic and Temporal Heterogeneity Within CD8+ T Cell Responses.

Review 1. Divide and Conquer: Phenotypic and Temporal Heterogeneity Within CD8⁺ T Cell Responses.