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3 results on '"Víctor, Collado-Díaz"'

1. Abacavir Increases Purinergic P2X7 Receptor Activation by ATP: Does a Pro-inflammatory Synergism Underlie Its Cardiovascular Toxicity?

Author

Víctor Collado-Díaz, Maria Ángeles Martinez-Cuesta, Maria Amparo Blanch-Ruiz, Ainhoa Sánchez-López, Patricia García-Martínez, José E Peris, Iris Usach, Maria Dolores Ivorra, Alessandra Lacetera, Sonsoles Martín-Santamaría, Juan V. Esplugues, and Angeles Alvarez

Subjects
abacavir, adenosine triphosphate, P2X7 receptor, leukocyte-endothelium interactions, cardiovascular diseases, allosteric modulator, Therapeutics. Pharmacology, RM1-950
Abstract

The cardiovascular toxicity of Abacavir is related to its purinergic structure. Purinergic P2X7-receptors (P2X7R), characterized by activation by high concentrations of ATP and with high plasticity, seem implicated. We appraise the nature of the interplay between Abacavir and P2X7R in generating vascular inflammation. The effects of Abacavir on leukocyte-endothelium interactions were compared with those of its metabolite carbovir triphosphate (CBV-TP) or ATP in the presence of apyrase (ATP-ase) or A804598 (P2X7R-antagonist). CBV-TP and ATP levels were evaluated by HPLC, while binding of Abacavir, CBV-TP and ATP to P2X7R was assessed by radioligand and docking studies. Hypersensitivity studies explored a potential allosteric action of Abacavir. Clinical concentrations of Abacavir (20 µmol/L) induced leukocyte-endothelial cell interactions by specifically activating P2X7R, but the drug did not show affinity for the P2X7R ATP-binding site (site 1). CBV-TP levels were undetectable in Abacavir-treated cells, while those of ATP were unaltered. The effects of Abacavir were Apyrase-dependent, implying dependence on endogenous ATP. Exogenous ATP induced a profile of proinflammatory actions similar to Abacavir, but was not entirely P2X7R-dependent. Docking calculations suggested ATP-binding to sites 1 and 2, and Abacavir-binding only to allosteric site 2. A combination of concentrations of Abacavir (1 µmol/L) and ATP (0.1 µmol/L) that had no effect when administered separately induced leukocyte-endothelium interactions mediated by P2X7R and involving Connexin43 channels. Therefore, Abacavir acts as a positive allosteric modulator of P2X7R, turning low concentrations of endogenous ATP themselves incapable of stimulating P2X7R into a functional proinflammatory agonist of the receptor.

Published
2021
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3. Abacavir causes leukocyte/platelet crosstalk by neutrophil P2X7 receptor release of sLOX-1

Author

Maria Amparo, Blanch-Ruíz, Ainhoa, Sánchez-López, César, Ríos-Navarro, Raquel, Ortega-Luna, Víctor, Collado-Díaz, Samuel, Orden, María Angeles, Martínez-Cuesta, Juan V, Esplugues, and Angeles, Alvarez

Abstract

Abacavir (ABC) - antiretroviral drug used in HIV-therapy and associated with myocardial infarction - promotes thrombosis through purinergic P2X7R. The role of platelets as pro-thrombotic cells is acknowledged while that of neutrophils - due to their secretory capacity - is gaining recognition. This study analyses the role of neutrophils - specifically the secretome of ABC-treated neutrophils (SNThe effects of ABC or SNABC induced platelet-leukocyte interactions, a consequence not of a direct effect of ABC on platelets, but rather the activation of neutrophils, which triggered an interplay between platelet P-selectin and neutrophil PSGL-1. SNNeutrophils are target cells in ABC-induced thrombosis. ABC acts on neutrophil P2X7R, inducing the release of sLOX-1, which in turn activates platelets. Hence, sLOX-1 could be the missing link in the cardiovascular risk associated with ABC.

Published
2022

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