Retrograde and Anterograde Transport of Lat-Vesicles during the Immunological Synapse Formation: Defining the Finely-Tuned Mechanism

LAT is an important player of the signaling cascade induced by TCR activation. This adapter molecule is present at the plasma membrane of T lymphocytes and more abundantly in intracellular compartments. Upon T cell activation the intracellular pool of LAT is recruited to the immune synapse (IS). We...

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Published inCells (Basel, Switzerland) Vol. 10; no. 2; p. 359
Main Authors Saez, Juan José, Dogniaux, Stephanie, Shafaq-Zadah, Massiullah, Johannes, Ludger, Hivroz, Claire, Zucchetti, Andrés Ernesto
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 09.02.2021
MDPI
Subjects
Anterograde transport
Antibodies
Cell activation
Endocytosis
Endosomes
Glycerol
Golgi apparatus
immune synapse
Immunological synapses
Intracellular
LAT
Life Sciences
Lymphocytes
Lymphocytes T
Plasmids
Protein transport
Proteins
Retrograde transport
Signal transduction
SNAP receptors
Syntaxin
T cell receptors
T-cell activation
St Louis Missouri
United Kingdom > UK
France
United States > US
immune synapse
LAT
T-cell activation
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Summary:LAT is an important player of the signaling cascade induced by TCR activation. This adapter molecule is present at the plasma membrane of T lymphocytes and more abundantly in intracellular compartments. Upon T cell activation the intracellular pool of LAT is recruited to the immune synapse (IS). We previously described two pathways controlling LAT trafficking: retrograde transport from endosomes to the TGN, and anterograde traffic from the Golgi to the IS. We address the specific role of four proteins, the GTPase Rab6, the t-SNARE syntaxin-16, the v-SNARE VAMP7 and the golgin GMAP210, in each pathway. Using different methods (endocytosis and Golgi trap assays, confocal and TIRF microscopy, TCR-signalosome pull down) we show that syntaxin-16 is regulating the retrograde transport of LAT whereas VAMP7 is regulating the anterograde transport. Moreover, GMAP210 and Rab6, known to contribute to both pathways, are in our cellular context, specifically and respectively, involved in anterograde and retrograde transport of LAT. Altogether, our data describe how retrograde and anterograde pathways coordinate LAT enrichment at the IS and point to the Golgi as a central hub for the polarized recruitment of LAT to the IS. The role that this finely-tuned transport of signaling molecules plays in T-cell activation is discussed.
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PMCID: PMC7916135
ISSN:2073-4409
2073-4409
DOI:10.3390/cells10020359