Please use this identifier to cite or link to this item: https://www.um.edu.mt/library/oar/handle/123456789/132134
Title: Clathrin mediates both internalization and vesicular release of triggered T cell receptor at the immunological synapse
Authors: Kvalvaag, Audun
Valvo, Salvatore
Céspedes, Pablo F.
Saliba, David
Kurz, Elke
Korobchevskaya, Kseniya
Dustin, Michael L.
Keywords: Lipids -- Physiological transport
Immunological synapses
Clathrin-coated vesicles
T cells -- Receptors
Endocytosis
Issue Date: 2023
Publisher: National Academy of Sciences
Citation: Kvalvaag, A., Valvo, S., Céspedes, P. F., Saliba, D. G., Kurz, E., Korobchevskaya, K., & Dustin, M. L. (2023). Clathrin mediates both internalization and vesicular release of triggered T cell receptor at the immunological synapse. Proceedings of the National Academy of Sciences, 120(6), e2211368120.
Abstract: Ligation of T cell receptor (TCR) to peptide–MHC (pMHC) complexes initiates signaling leading to T cell activation and TCR ubiquitination. Ubiquitinated TCR is then either internalized by the T cell or released toward the antigen-presenting cell (APC) in extracellular vesicles. How these distinct fates are orchestrated is unknown. Here, we show that clathrin is first recruited to TCR microclusters by HRS and STAM2 to initiate release of TCR in extracellular vesicles through clathrin- and ESCRT-mediated ectocytosis directly from the plasma membrane. Subsequently, EPN1 recruits clathrin to remaining TCR microclusters to enable trans-endocytosis of pMHC–TCR conjugates from the APC. With these results, we demonstrate how clathrin governs bidirectional membrane exchange at the immunological synapse through two topologically opposite processes coordinated by the sequential recruitment of ecto- and endocytic adaptors. This provides a scaffold for direct two-way communication between T cells and APCs.
URI: https://www.um.edu.mt/library/oar/handle/123456789/132134
Appears in Collections:Scholarly Works - FacHScABS



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