Litcius/Paper detail

A Comprehensive Tyrosine Phosphoproteomic Analysis Reveals Novel Components of the Platelet CLEC-2 Signaling Cascade

Irene Izquierdo, María N. Barrachina, Lidia Hermida‐Nogueira, Vanessa Casas, Luis A. Morán, Serena Lacerenza, Roberto Pinto-Llorente, Johannes A. Eble, Vivian de los Rı́os, Eduardo Domínguez, Marı́a Isabel Loza, J. Ignacio Casal, Montserrat Carrascal, Joaquín Abián, Ángel Galindo García

2020Thrombosis and Haemostasis27 citationsDOI

Abstract

Abstract C-type lectin-like receptor 2 (CLEC-2) plays a crucial role in different platelet-related physiological and pathological processes. It signals through a tyrosine kinase-mediated pathway that is highly dependent on the positive feedback exerted by the platelet-derived secondary mediators, adenosine diphosphate (ADP) and thromboxane A2 (TXA2). Here, we aimed to analyze the tyrosine phosphoproteome of platelets activated with the CLEC-2 agonist rhodocytin to identify relevant phosphorylated tyrosine residues (p-Tyr) and proteins involved in platelet activation downstream of this receptor. We identified 363 differentially p-Tyr residues, corresponding to the majority of proteins previously known to participate in CLEC-2 signaling and also novel ones, including adaptors (e.g., DAPP1, Dok1/3, CASS4, Nck1/2), kinases/phosphatases (e.g., FAK1, FES, FGR, JAK2, SHIP2), and membrane proteins (e.g., G6F, JAM-A, PECAM-1, TLT-1). To elucidate the contribution of ADP and TXA2 at different points of the CLEC-2 signaling cascade, we evaluated p-Tyr levels of residues identified in the analysis and known to be essential for the catalytic activity of kinases Syk(p-Tyr525+526) and Src(p-Tyr419), and for PLCγ2 activity (p-Tyr759). We demonstrated that Syk phosphorylation at Tyr525+526 also happens in the presence of ADP and TXA2 inhibitors, which is not the case for Src-pTyr419 and PLCγ2-pTyr759. Kinetics studies for the three phosphoproteins show some differences in the phosphorylation profile. Ca2+ mobilization assays confirmed the relevance of ADP and TXA2 for full CLEC-2-mediated platelet activation. The present study provides significant insights into the intracellular events that take place following CLEC-2 activation in platelets, contributing to elucidate in detail the CLEC-2 signalosome.

Topics & Concepts

SykPhosphorylationProto-oncogene tyrosine-protein kinase SrcPlatelet activationTyrosine phosphorylationThromboxane A2Cell biologyProtein tyrosine phosphataseChemistryTyrosineKinaseSignal transductionTyrosine kinasePlateletBiochemistrySH2 domainAdenosine diphosphateReceptor tyrosine kinaseReceptorBiologyImmunologyPlatelet aggregationPlatelet Disorders and TreatmentsMast cells and histamineCell Adhesion Molecules Research