Insights into the allosteric regulation of Syk association with receptor ITAM, a multi-state equilibrium

Feng, Chao; Post, Carol Beth

doi:10.1039/c5cp05417f

Cited by 15 publications

(51 citation statements)

References 46 publications

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“…4). In particular, there is a decrease in the number of contacts between the N-SH2 and C-SH2 domains in the presence of the mutation, which is consistent with the experimentally-observed partial decoupling of both SH2 domains in the mutant (Zhang et al, 2008;Feng and Post, 2016;Roy et al, 2016).…”

Section: Discussionsupporting

confidence: 85%

“…MD simulations provided insufficient information on the influence of the Y130E substitution on helical stability, due to limited sampling even at microsecond time scales. Motivated by experimental observations that Y130E does disrupt helical stability (Zhang et al, 2008;Feng and Post, 2016;Roy et al, 2016), we computed inter-SH2 distance distribution from REMD simulations of the interdomain A linker. Only the linker was included in these simulations in order to enhance the sampling of adopted conformations and to evaluate the impact of the Y130E mutation.…”

Section: Discussionmentioning

confidence: 99%

“…We specially focus on Syk recruitment after phosphorylation at site Y130 in interdomain A (Keshvara et al, 1998), since Y130E substitution in Syk resulted in a phosphomimetic recombinant protein with reduced binding of its tandem SH2 domains to phosphorylated ITAMs in co-immunoprecipitation studies (Keshvara et al, 1997;Zhang et al, 2008). This was initially attributed to the structural destabilization of interdomain A and the resulting partial decoupling of both SH2 domains (Zhang et al, 2008;Feng and Post, 2016;Roy et al, 2016). However, high resolution imaging studies in Syk-deficient cells reconstituted with Syk Y130E recombinant protein revealed two interesting observations: 1) Syk recruitment to FcεRI aggregates is retained even for Y130E phosphomimetic, and 2) impaired downstream signaling correlates with an increased off-rate for FcεRI-Syk-Y130E interactions (Schwartz et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

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Molecular aspects of multivalent engagement between Syk and FcεRIγ

Travers

Kanagy

Jhamba

et al. 2018

Preprint

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Syk/Zap70 family kinases are essential for signaling via multichain immune-recognition receptors such as the tetrameric (αβγ2) FcεRI. The simplest model assumes that Syk activation occurs through cis binding of its tandem SH2 domains to dual phosphotyrosines within immunoreceptor tyrosine-based activation motifs of individual γ chains. In this model, Syk activity is modulated by phosphorylation occurring between adjacent Syk molecules docked on γ homodimers and by Lyn molecules bound to FcεRIβ. However, the mechanistic details of Syk docking on γ homodimers are not fully resolved, particularly the possibility of trans binding orientations and the impact of Y130 autophosphorylation within Syk interdomain A. Analytical modeling shows that multivalent interactions lead to increased WT Syk cis-oriented binding by three orders of magnitude. Molecular dynamics (MD) simulations show increased inter-SH2 flexibility in a Y130Ephosphomimetic form of Syk, associated with reduced overall helicity of interdomain A. Hybrid MD/worm-like chain polymer models show that the Y130E substitution reduces cis binding of Syk. We report computational models and estimates of relative binding for all possible cis and trans 2:2 Syk:FcεRIγ complexes. Calcium imaging experiments confirm model predictions that cis binding of WT Syk is strongly preferred for efficient signaling, while trans conformations trigger weak but measurable responses.

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Section: Discussionsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Molecular aspects of multivalent engagement between Syk and FcεRIγ

Travers

Kanagy

Jhamba

et al. 2018

Preprint

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“…The importance of the longer-lived interactions in signal propagation is shown by introduction of a Y130E mutation within the I-A domain of Syk. Phosphorylation of Y130 is proposed as a form of negative-feedback regulation, because it has been shown to destabilize binding of Syk tandem SH2 domains to phosphorylated ITAMs (pITAMs) ( Zhang et al , 2008 ; Feng and Post, 2016 ). We find that Syk-Y130E is still recruited to FcεRI aggregates, but its interactions are more transient ( k s = 0.87 s −1 ) and markedly less efficient at transphosphorylation.…”

Section: Introductionmentioning

confidence: 99%

Differential mast cell outcomes are sensitive to FcεRI-Syk binding kinetics

Schwartz

Cleyrat

Olah

et al. 2017

MBoC

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“…The importance of the longer-lived interactions in signal propagation is shown by introduction of a Y130E mutation within the I-A domain of Syk. Phosphorylation of Y130 is proposed as a form of negative feedback regulation since it has been shown to destabilize binding of Syk tandem SH2 domains to phosphorylated ITAMs (pITAM) (Feng and Post, 2015;Zhang et al, 2008). We find that Syk-Y130E is still recruited to FcRI aggregates, but its interactions are more transient (ks = 0.87 s -1 ) and markedly less efficient at transphosphorylation.…”

Section: Introductionmentioning

confidence: 82%