Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling

SLAM family receptors regulate activation and inhibition in immunity through recruitment of activating and inhibitory SH2 domain containing proteins to immunoreceptor tyrosine based switch motifs (ITSMs). Binding of the adaptors, SAP and EAT-2 to ITSMs in the cytoplasmic regions of SLAM family recep...

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Autores principales: Wilson, Timothy J., Garner, Lee I., Metcalfe, Clive, King, Elliott, Margraf, Stefanie, Brown, Marion H.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3958483/
https://www.ncbi.nlm.nih.gov/pubmed/24642916
http://dx.doi.org/10.1371/journal.pone.0092184
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author Wilson, Timothy J.
Garner, Lee I.
Metcalfe, Clive
King, Elliott
Margraf, Stefanie
Brown, Marion H.
author_facet Wilson, Timothy J.
Garner, Lee I.
Metcalfe, Clive
King, Elliott
Margraf, Stefanie
Brown, Marion H.
author_sort Wilson, Timothy J.
collection PubMed
description SLAM family receptors regulate activation and inhibition in immunity through recruitment of activating and inhibitory SH2 domain containing proteins to immunoreceptor tyrosine based switch motifs (ITSMs). Binding of the adaptors, SAP and EAT-2 to ITSMs in the cytoplasmic regions of SLAM family receptors is important for activation. We analysed the fine specificity of SLAM family receptor phosphorylated ITSMs and the conserved tyrosine motif in EAT-2 for SH2 domain containing signalling proteins. Consistent with the literature describing dependence of CRACC (SLAMF7) on EAT-2, CRACC bound EAT-2 (K(D) = 0.003 μM) with approximately 2 orders of magnitude greater affinity than SAP (K(D) = 0.44 μM). RNA interference in cytotoxicity assays in NK92 cells showed dependence of CRACC on SAP in addition to EAT-2, indicating selectivity of SAP and EAT-2 may depend on the relative concentrations of the two adaptors. The concentration of SAP was four fold higher than EAT-2 in NK92 cells. Compared with SAP, the significance of EAT-2 recruitment and its downstream effectors are not well characterised. We identified PLCγ1 and PLCγ2 as principal binding partners for the EAT-2 tail. Both PLCγ1 and PLCγ2 are functionally important for cytotoxicity in NK92 cells through CD244 (SLAMF4), NTB-A (SLAMF6) and CRACC. Comparison of the specificity of SH2 domains from activating and inhibitory signalling mediators revealed a hierarchy of affinities for CD244 (SLAMF4) ITSMs. While binding of phosphatase SH2 domains to individual ITSMs of CD244 was weak compared with SAP or EAT-2, binding of tandem SH2 domains of SHP-2 to longer peptides containing tandem phosphorylated ITSMs in human CD244 increased the affinity ten fold. The concentration of the tyrosine phosphatase, SHP-2 was in the order of a magnitude higher than the adaptors, SAP and EAT-2. These data demonstrate a mechanism for direct recruitment of phosphatases in inhibitory signalling by ITSMs, while explaining competitive dominance of SAP and EAT-2.
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spelling pubmed-39584832014-03-24 Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling Wilson, Timothy J. Garner, Lee I. Metcalfe, Clive King, Elliott Margraf, Stefanie Brown, Marion H. PLoS One Research Article SLAM family receptors regulate activation and inhibition in immunity through recruitment of activating and inhibitory SH2 domain containing proteins to immunoreceptor tyrosine based switch motifs (ITSMs). Binding of the adaptors, SAP and EAT-2 to ITSMs in the cytoplasmic regions of SLAM family receptors is important for activation. We analysed the fine specificity of SLAM family receptor phosphorylated ITSMs and the conserved tyrosine motif in EAT-2 for SH2 domain containing signalling proteins. Consistent with the literature describing dependence of CRACC (SLAMF7) on EAT-2, CRACC bound EAT-2 (K(D) = 0.003 μM) with approximately 2 orders of magnitude greater affinity than SAP (K(D) = 0.44 μM). RNA interference in cytotoxicity assays in NK92 cells showed dependence of CRACC on SAP in addition to EAT-2, indicating selectivity of SAP and EAT-2 may depend on the relative concentrations of the two adaptors. The concentration of SAP was four fold higher than EAT-2 in NK92 cells. Compared with SAP, the significance of EAT-2 recruitment and its downstream effectors are not well characterised. We identified PLCγ1 and PLCγ2 as principal binding partners for the EAT-2 tail. Both PLCγ1 and PLCγ2 are functionally important for cytotoxicity in NK92 cells through CD244 (SLAMF4), NTB-A (SLAMF6) and CRACC. Comparison of the specificity of SH2 domains from activating and inhibitory signalling mediators revealed a hierarchy of affinities for CD244 (SLAMF4) ITSMs. While binding of phosphatase SH2 domains to individual ITSMs of CD244 was weak compared with SAP or EAT-2, binding of tandem SH2 domains of SHP-2 to longer peptides containing tandem phosphorylated ITSMs in human CD244 increased the affinity ten fold. The concentration of the tyrosine phosphatase, SHP-2 was in the order of a magnitude higher than the adaptors, SAP and EAT-2. These data demonstrate a mechanism for direct recruitment of phosphatases in inhibitory signalling by ITSMs, while explaining competitive dominance of SAP and EAT-2. Public Library of Science 2014-03-18 /pmc/articles/PMC3958483/ /pubmed/24642916 http://dx.doi.org/10.1371/journal.pone.0092184 Text en © 2014 Wilson et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wilson, Timothy J.
Garner, Lee I.
Metcalfe, Clive
King, Elliott
Margraf, Stefanie
Brown, Marion H.
Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title_full Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title_fullStr Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title_full_unstemmed Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title_short Fine Specificity and Molecular Competition in SLAM Family Receptor Signalling
title_sort fine specificity and molecular competition in slam family receptor signalling
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3958483/
https://www.ncbi.nlm.nih.gov/pubmed/24642916
http://dx.doi.org/10.1371/journal.pone.0092184
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