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CXCL12 Regulates through JAK1 and JAK2 Formation of Productive Immunological Synapses.

J Immunol. 2015; 
Cascio G, Martín-Cófreces NB, Rodríguez-Frade JM, López-Cotarelo P, Criado G, Pablos JL, Rodríguez-Fernández JL, Sánchez-Madrid F, Mellado M.
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Peptide Synthesis Briefly, matured BM-DC (1 mg/ml LPS, 12 h, 37˚C) were loaded with OVA323–339-peptide (5 mM, 30 min, 37˚C; GenScript) and mixed in complete medium (RPMI 1640 medium, 10% FCS) with CD4+ T cells (1:5 DC:CD4+ T cells). Get A Quote

摘要

The adaptive immune response requires interaction between T cells and APC to form a specialized structure termed the immune synapse (IS). Although the TCR is essential for IS organization, other factors such as chemokines participate in this process. In this study, we show that the chemokine CXCL12-mediated signaling contributes to correct IS organization and therefore influences T cell activation. CXCR4 downregulation or blockade on T cells caused defective actin polymerization at the contact site with APC, altered microtubule-organizing center polarization and the IS structure, and reduced T cell/APC contact duration. T cell activation was thus inhibited, as shown by reduced expression of CD25 and CD69 marker... More

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