The chaperonin CCT controls T cell receptor-driven 3D configuration of centrioles.
Noa Beatriz Martín-CófrecesFrancisco Javier ChichónEnrique CalvoDaniel TorralbaEugenio Bustos-MoránSara G DosilAmelia Rojas-GomezElena Bonzón-KulichenkoJuan Antonio LópezJoaquin OtónAndrea SorrentinoJ C ZabalaIsabelle VernosJesus VazquezJosé María ValpuestaFrancisco Sánchez-MadridPublished in: Science advances (2020)
T lymphocyte activation requires the formation of immune synapses (IS) with antigen-presenting cells. The dynamics of membrane receptors, signaling scaffolds, microfilaments, and microtubules at the IS determine the potency of T cell activation and subsequent immune response. Here, we show that the cytosolic chaperonin CCT (chaperonin-containing TCP1) controls the changes in reciprocal orientation of the centrioles and polarization of the tubulin dynamics induced by T cell receptor in T lymphocytes forming an IS. CCT also controls the mitochondrial ultrastructure and the metabolic status of T cells, regulating the de novo synthesis of tubulin as well as posttranslational modifications (poly-glutamylation, acetylation, Δ1 and Δ2) of αβ-tubulin heterodimers, fine-tuning tubulin dynamics. These changes ultimately determine the function and organization of the centrioles, as shown by three-dimensional reconstruction of resting and stimulated primary T cells using cryo-soft x-ray tomography. Through this mechanism, CCT governs T cell activation and polarity.