Abacavir induces platelet-endothelium interactions by interfering with purinergic signalling: A step from inflammation to thrombosis.

6533b82dfe1ef96bd1291556

RESEARCH PRODUCT

Abacavir induces platelet-endothelium interactions by interfering with purinergic signalling: A step from inflammation to thrombosis.

Cesar Rios-navarro Samuel Orden M. A. Martínez-cuesta ÁNgeles ÁLvarez Juan V. Esplugues Isabel Andújar Victor Collado-diaz María Amparo Blanch-ruiz

subject

0301 basic medicine Blood Platelets Endothelium Platelet Aggregation Anti-HIV Agents Inflammation Pharmacology Biology Proinflammatory cytokine 03 medical and health sciences 0302 clinical medicine Platelet Adhesiveness platelet-endothelium interactions Virology medicine Humans Platelet 030212 general & internal medicine Platelet activation Pharmacology Inflammation Cell adhesion molecule Purinergic receptor Deoxyguanine Nucleotides Thrombosis Purinergic signalling Intercellular Adhesion Molecule-1 Platelet Activation Abacavir NRTIs Dideoxynucleosides Cell biology cardiovascular diseases P-Selectin 030104 developmental biology medicine.anatomical_structure Cardiovascular Diseases Purines Endothelium Vascular medicine.symptom Signal Transduction

description

The controversy connecting Abacavir (ABC) with cardiovascular disease has been fuelled by the lack of a credible mechanism of action. ABC shares structural similarities with endogenous purines, signalling molecules capable of triggering prothrombotic/proinflammatory programmes. Platelets are leading actors in the process of thrombosis. Our study addresses the effects of ABC on interactions between platelets and other vascular cells, while exploring the adhesion molecules implicated and the potential interference with the purinergic signalling pathway. The effects of ABC on platelet aggregation and platelet-endothelium interactions were evaluated, respectively, with an aggregometer and a flow chamber system that reproduced conditions in vivo. The role of adhesion molecules and purinergic receptors in endothelial and platelet populations was assessed by selective pre-incubation with specific antagonists and antibodies. ABC and carbovir triphosphate (CBT) levels were evaluated by HPLC. The results showed that ABC promoted the adherence of platelets to endothelial cells, a crucial step for the formation of thrombi. This was not a consequence of a direct effect of ABC on platelets, but resulted from activation of the endothelium via purinergic ATP-P2X7 receptors, which subsequently triggered an interplay between P-selectin and ICAM-1 on endothelial cells with constitutively expressed GPIIb/IIIa and GPIbα on platelets. ABC did not induce platelet activation (P-selectin expression or Ca2+ mobilization) or aggregation, even at high concentrations. CBT levels in endothelial cells were lower than those required to induce platelet-endothelium interactions. Thus, ABC interference with endothelial purinergic signalling leads to platelet recruitment. This highlights the endothelium as the main cell target of ABC in this interaction, which is in line with previous experimental evidence that ABC induces manifestations of vascular inflammation.

year	journal	country	edition	language
2017-05-01	Antiviral research

10.1016/j.antiviral.2017.03.001 https://pubmed.ncbi.nlm.nih.gov/28263802