[PDF][PDF] Activation-induced polarized recycling targets T cell antigen receptors to the immunological synapse: involvement of SNARE complexes

V Das, B Nal, A Dujeancourt, MI Thoulouze, T Galli… - Immunity, 2004 - cell.com
V Das, B Nal, A Dujeancourt, MI Thoulouze, T Galli, P Roux, A Dautry-Varsat, A Alcover
Immunity, 2004cell.com
The mechanism by which T cell antigen receptors (TCR) accumulate at the immunological
synapse has not been fully elucidated. Since TCRs are continuously internalized and
recycled back to the cell surface, we investigated the role of polarized recycling in TCR
targeting to the immunological synapse. We show here that the recycling endosomal
compartment of T cells encountering activatory antigen-presenting cells (APCs) polarizes
towards the T cell-APC contact site. Moreover, TCRs in transit through recycling endosomes …
Abstract
The mechanism by which T cell antigen receptors (TCR) accumulate at the immunological synapse has not been fully elucidated. Since TCRs are continuously internalized and recycled back to the cell surface, we investigated the role of polarized recycling in TCR targeting to the immunological synapse. We show here that the recycling endosomal compartment of T cells encountering activatory antigen-presenting cells (APCs) polarizes towards the T cell-APC contact site. Moreover, TCRs in transit through recycling endosomes are targeted to the immunological synapse. Inhibition of T cell polarity, constitutive TCR endocytosis, or recycling reduces TCR accumulation at the immunological synapse. Conversely, increasing the amount of TCRs in recycling endosomes before synapse formation enhanced their accumulation. Finally, we show that exocytic t-SNAREs from T cells cluster at the APC contact site and that tetanus toxin inhibits TCR accumulation at the immunological synapse, indicating that vesicle fusion mediated by SNARE complexes is involved in TCR targeting to the immunological synapse.
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