Frontiers in Immunology (Apr 2019)

Protein Kinase C δ Regulates the Depletion of Actin at the Immunological Synapse Required for Polarized Exosome Secretion by T Cells

  • Gonzalo Herranz,
  • Pablo Aguilera,
  • Sergio Dávila,
  • Alicia Sánchez,
  • Bianca Stancu,
  • Jesús Gómez,
  • David Fernández-Moreno,
  • Raúl de Martín,
  • Mario Quintanilla,
  • Teresa Fernández,
  • Pablo Rodríguez-Silvestre,
  • Laura Márquez-Expósito,
  • Ana Bello-Gamboa,
  • Alberto Fraile-Ramos,
  • Víctor Calvo,
  • Manuel Izquierdo

DOI
https://doi.org/10.3389/fimmu.2019.00851
Journal volume & issue
Vol. 10

Abstract

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Multivesicular bodies (MVB) are endocytic compartments that enclose intraluminal vesicles (ILVs) formed by inward budding from the limiting membrane of endosomes. In T lymphocytes, ILVs are secreted as Fas ligand-bearing, pro-apoptotic exosomes following T cell receptor (TCR)-induced fusion of MVB with the plasma membrane at the immune synapse (IS). In this study we show that protein kinase C δ (PKCδ), a novel PKC isotype activated by diacylglycerol (DAG), regulates TCR-controlled MVB polarization toward the IS and exosome secretion. Concomitantly, we demonstrate that PKCδ-interfered T lymphocytes are defective in activation-induced cell death. Using a DAG sensor based on the C1 DAG-binding domain of PKCδ and a GFP-PKCδ chimera, we reveal that T lymphocyte activation enhances DAG levels at the MVB endomembranes which mediates the association of PKCδ to MVB. Spatiotemporal reorganization of F-actin at the IS is inhibited in PKCδ-interfered T lymphocytes. Therefore, we propose PKCδ as a DAG effector that regulates the actin reorganization necessary for MVB traffic and exosome secretion.

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