2018
DOI: 10.1073/pnas.1817142115
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Cooperative assembly of a four-molecule signaling complex formed upon T cell antigen receptor activation

Abstract: The T cell antigen receptor encounters foreign antigen during the immune response. Receptor engagement leads to activation of specific protein tyrosine kinases, which then phosphorylate multiple enzymes and adapter proteins. One such enzyme, phospholipase-Cγ1, is responsible for cleavage of a plasma membrane lipid substrate, a phosphoinositide, into two second messengers, diacylglycerol, which activates several enzymes including protein kinase C, and an inositol phosphate, which induces intracellular calcium e… Show more

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Cited by 23 publications
(27 citation statements)
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“…Assembly of the LAT signalosome appears to be driven by multiple cooperative binding events, including, but not limited to Gads dimerization. A recent study highlighted the cooperative assembly of LAT, Gads, SLP-76, and PLC-γ1 into a tetrameric complex centered around LAT Tyr 132 and Tyr 171 (46). Upon in vitro reconstitution of this binding complex, elimination of any one of the above components reduced the binding interactions between the other three.…”
Section: The Regulated Assembly and Disassembly Of Lat-nucleated Signmentioning
confidence: 99%
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“…Assembly of the LAT signalosome appears to be driven by multiple cooperative binding events, including, but not limited to Gads dimerization. A recent study highlighted the cooperative assembly of LAT, Gads, SLP-76, and PLC-γ1 into a tetrameric complex centered around LAT Tyr 132 and Tyr 171 (46). Upon in vitro reconstitution of this binding complex, elimination of any one of the above components reduced the binding interactions between the other three.…”
Section: The Regulated Assembly and Disassembly Of Lat-nucleated Signmentioning
confidence: 99%
“…One possible compensatory mechanism is the Gads-independent recruitment of SLP-76 to LAT by other Grb2-family members, Grb2 or Grap. Both Gads and Grb2 can bind via their C-terminal SH3 domains to a non-canonical RxxK motif found in SLP-76; however, Gads binds this motif with high affinity, measured at 9-20 nM (8, 10, 46), whereas Grb2 binds with ~500-fold lower affinity (10, 14, 15). Due to its low affinity, Grb2 cannot interact with SLP-76 in the presence of competing Gads (18); however, the absence of Gads may permit weak, Grb2-mediated recruitment of SLP-76 to LAT.…”
Section: Can We Solve the Puzzle Of Gads?mentioning
confidence: 99%
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“…PLC1 is a multi-domain lipase. Besides its catalytic core, PLC1 also contains two SH2 domains and one SH3 domain that serve structural or regulatory roles (Braiman et al, 2006;Manna et al, 2018). Its N-terminal SH2 domain (nSH2) binds specifically to phosphor-tyrosine (Y132) on LAT (Braiman et al, 2006) whereas its C-terminal SH2 domain (cSH2) is involved in releasing autoinhibition of PLC1 (Gresset et al, 2010;Hajicek et al, 2019).…”
Section: Introductionmentioning
confidence: 99%
“…The SH3 domain of PLC1 directly interacts with the proline-rich motifs on Sos1 (Kim et al, 2000), a RasGEF which is also enriched in the LAT microclusters. The multiple binary interactions between PLC1 and other components in the LAT complex mediate a synergistic assembly of the LAT complex (Braiman et al, 2006;Hartgroves et al, 2003;Manna et al, 2018). However, because of the complex protein-protein interactions involved, the exact mechanism of how PLC1 regulates LAT microcluster formation remains elusive.…”
Section: Introductionmentioning
confidence: 99%