AI Article Synopsis

  • - Antigen recognition by the T cell receptor leads to the formation of SLP-76 microclusters, essential for T cell signaling and stabilization of contacts.
  • - The interaction between the protein ADAP and SLP-76 supports the formation of persistent microclusters and promotes T cell adhesion and CD69 upregulation, highlighting ADAP's role in T cell activation.
  • - A specific phosphorylation site on ADAP (Y595) is crucial for its function, with phosphorylation affecting its interactions with SLP-76 and enhancing the stability of the signaling complexes in T cells.

Article Abstract

Antigen recognition by the T cell receptor (TCR) directs the assembly of essential signaling complexes known as SLP-76 (also known as LCP2) microclusters. Here, we show that the interaction of the adhesion and degranulation-promoting adaptor protein (ADAP; also known as FYB1) with SLP-76 enables the formation of persistent microclusters and the stabilization of T cell contacts, promotes integrin-independent adhesion and enables the upregulation of CD69. By analyzing point mutants and using a novel phospho-specific antibody, we show that Y595 is essential for normal ADAP function, that virtually all tyrosine phosphorylation of ADAP is restricted to a Y595-phosphorylated (pY595) pool, and that multivalent interactions between the SLP-76 SH2 domain and its binding sites in ADAP are required to sustain ADAP phosphorylation. Although pY595 ADAP enters SLP-76 microclusters, non-phosphorylated ADAP is enriched in protrusive actin-rich structures. The pre-positioning of ADAP at the contact sites generated by these structures favors the retention of nascent SLP-76 oligomers and their assembly into persistent microclusters. Although ADAP is frequently depicted as an effector of SLP-76, our findings reveal that ADAP acts upstream of SLP-76 to convert labile, Ca-competent microclusters into stable adhesive junctions with enhanced signaling potential.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6240300PMC
http://dx.doi.org/10.1242/jcs.215517DOI Listing

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