AI Article Synopsis

  • The SH2 domain containing leukocyte protein (SLP) adaptor proteins play a key role in helping lymphocytes respond to antigens by organizing important signaling protein complexes.
  • In T cells, SLP-76 forms a large complex (about 400 kDa) with Gads, while in B cells, SLP-65 exists in both a 180 kDa complex and a monomeric state.
  • After antigen stimulation, only the complexed SLP-65 is phosphorylated, but the study indicates that active signaling complexes are temporary and exist in low amounts.

Article Abstract

SH2 domain containing leukocyte protein (SLP) adaptor proteins serve a central role in the antigen-mediated activation of lymphocytes by organizing multiprotein signaling complexes. Here, we use two dimensional native-/SDS-gel electrophoresis to study the number, size and relative abundance of protein complexes containing SLP family proteins. In non-stimulated T cells all SLP-76 proteins are in a approximately 400 kDa complex with the small adaptor protein Grb2-like adaptor protein downstream of Shc (Gads), whereas half of Gads is monomeric. This constitutive SLP-76/Gads complex could be reconstituted in Drosophila S2 cells expressing both components, suggesting that it might not contain additional subunits. In contrast, in B cells SLP-65 exists in a 180 kDa complex as well as in monomeric form. Since the complex was not found in S2 cells expressing only SLP-65, it was not di/trimeric SLP-65. Upon antigen-stimulation only the complexed SLP-65 was phosphorylated. Surprisingly, stimulation-induced alteration of SLP complexes could not be detected, suggesting that active signaling complexes form only transiently, and are of low abundance.

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http://dx.doi.org/10.1016/j.imlet.2005.11.004DOI Listing

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