Systems-level conservation of the proximal TCR signaling network of mice and humans

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Nicolas, Philippe | Ollier, Jocelyn | Mori, Daiki | Voisinne, Guillaume | Celis-Gutierrez, Javier | Gregoire, Claude | Perroteau, Jeanne | Vivien, Régine | Camus, Mylène | Burlet-Schiltz, Odile | Gonzalez de Peredo, Anne | Clémenceau, Béatrice | Roncagalli, Romain | Vié, Henri | Malissen, Bernard

Edité par CCSD ; Rockefeller University Press -

International audience. We exploited traceable gene tagging in primary human T cells to establish the composition and dynamics of seven canonical TCR-induced protein signaling complexes (signalosomes) using affinity purification coupled with mass spectrometry (AP-MS). It unveiled how the LAT adaptor assembles higher-order molecular condensates and revealed that the proximal TCR-signaling network has a high degree of qualitative and quantitative conservation between human CD4 + and CD8 + T cells. Such systemslevel conservation also extended across human and mouse T cells and unexpectedly encompassed protein-protein interaction stoichiometry. Independently of evolutionary considerations, our study suggests that a drug targeting the proximal TCR signaling network should behave similarly when applied to human and mouse T cells. However, considering that signaling differences likely exist between the distal TCR-signaling pathway of human and mouse, our fast-track AP-MS approach should be favored to determine the mechanism of action of drugs targeting human T cell activation. An opportunity is illustrated here using an inhibitor of the LCK protein tyrosine kinase as a proof-of-concept.

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