AI Article Synopsis

  • TCR signaling microclusters are essential for T cell activation, with GPI-anchored proteins like CD48 playing a key role.
  • Upon T cell activation, CD48 is recruited to the TCR/CD3 complex, crucial for IL-2 production by linking early signaling component LAT to the complex.
  • CD2 acts as a master switch in this process, linking the Src kinase Lck to the CD48/LAT complex, thus facilitating the formation of the TCR signalosome.

Article Abstract

The buildup of TCR signaling microclusters containing adaptor proteins and kinases is prerequisite for T cell activation. One hallmark in this process is association of the TCR with lipid raft microdomains enriched in GPI-proteins that have potential to act as accessory molecules for TCR signaling. In this study, we show that GPI-anchored CD48 but not CD59 was recruited to the immobilized TCR/CD3 complex upon activation of T cells. CD48 reorganization was vital for T cell IL-2 production by mediating lateral association of the early signaling component linker for activated T cells (LAT) to the TCR/CD3 complex. Furthermore, we identified CD2 as an adaptor linking the Src protein tyrosine kinase Lck and the CD48/LAT complex to TCR/CD3: CD2 associated with TCR/CD3 upon T cell activation irrespective of CD48 expression, while association of CD48 and LAT with the TCR/CD3 complex depended on CD2. Consequently, our data indicate that CD2 and CD48 cooperate hierarchically in the buildup of the early TCR signalosome; CD2 functions as the master switch recruiting CD48 and Lck. CD48 in turn shuttles the transmembrane adapter molecule LAT.

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Source
http://dx.doi.org/10.4049/jimmunol.0800691DOI Listing

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