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Carbamylation of Integrin α IIb β 3: The Mechanistic Link to Platelet Dysfunction in ESKD

Veronika Binder, Barbara Chruścicka‐Smaga, Brith Bergum, Stéphane Jaisson, Philippe Gillery, Joar Sivertsen, Tor Hervig, Marta Kamińska, Ronak Tilvawala, Venkatesh V. Nemmara, Paul R. Thompson, Jan Potempa, Hans‐Peter Marti, Piotr Mydel

2022Journal of the American Society of Nephrology12 citationsDOIOpen Access PDF

Abstract

Background Bleeding diatheses, common among patients with ESKD, can lead to serious complications, particularly during invasive procedures. Chronic urea overload significantly increases cyanate concentrations in patients with ESKD, leading to carbamylation, an irreversible modification of proteins and peptides. Methods To investigate carbamylation as a potential mechanistic link between uremia and platelet dysfunction in ESKD, we used liquid chromatography-tandem mass spectrometry (HPLC-MS/MS) to quantify total homocitrulline, and biotin-conjugated phenylglyoxal labeling and Western blot to detect carbamylated integrin α IIb β 3 (a receptor required for platelet aggregation). Flow cytometry was used to study activation of isolated platelets and platelet-rich plasma. In a transient transfection system, we tested activity and fibrinogen binding of different mutated forms of the receptor. We assessed platelet adhesion and aggregation in microplate assays. Results Carbamylation inhibited platelet activation, adhesion, and aggregation. Patients on hemodialysis exhibited significantly reduced activation of α IIb β 3 compared with healthy controls. We found significant carbamylation of both subunits of α IIb β 3 on platelets from patients receiving hemodialysis versus only minor modification in controls. In the transient transfection system, modification of lysine 185 in the β 3 subunit was associated with loss of receptor activity and fibrinogen binding. Supplementation of free amino acids, which was shown to protect plasma proteins from carbamylation-induced damage in patients on hemodialysis, prevented loss of α IIb β 3 activity in vitro . Conclusions Carbamylation of α IIb β 3 —specifically modification of the K185 residue—might represent a mechanistic link between uremia and dysfunctional primary hemostasis in patients on hemodialysis. The observation that free amino acids prevented the carbamylation-induced loss of α IIb β 3 activity suggests amino acid administration during dialysis may help to normalize platelet function.

Topics & Concepts

PlateletChemistryUremiaFibrinogenIntegrinPlatelet activationBiochemistryInternal medicineReceptorMedicinePlatelet Disorders and TreatmentsBlood properties and coagulationCell Adhesion Molecules Research
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