Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus

Blood platelets’ adenosine receptors (AR) are considered to be a new target for the anti-platelet therapy. This idea is based on in vitro studies which show that signaling mediated by these receptors leads to a decreased platelet response to activating stimuli. In vivo evidence for the antithromboti...

Descripción completa

Detalles Bibliográficos
Autores principales: Polak, Dawid, Talar, Marcin, Wolska, Nina, Wojkowska, Dagmara W., Karolczak, Kamil, Kramkowski, Karol, Bonda, Tomasz A., Watala, Cezary, Przygodzki, Tomasz
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8002731/
https://www.ncbi.nlm.nih.gov/pubmed/33802928
http://dx.doi.org/10.3390/ijms22063074
_version_ 1783671532111790080
author Polak, Dawid
Talar, Marcin
Wolska, Nina
Wojkowska, Dagmara W.
Karolczak, Kamil
Kramkowski, Karol
Bonda, Tomasz A.
Watala, Cezary
Przygodzki, Tomasz
author_facet Polak, Dawid
Talar, Marcin
Wolska, Nina
Wojkowska, Dagmara W.
Karolczak, Kamil
Kramkowski, Karol
Bonda, Tomasz A.
Watala, Cezary
Przygodzki, Tomasz
author_sort Polak, Dawid
collection PubMed
description Blood platelets’ adenosine receptors (AR) are considered to be a new target for the anti-platelet therapy. This idea is based on in vitro studies which show that signaling mediated by these receptors leads to a decreased platelet response to activating stimuli. In vivo evidence for the antithrombotic activity of AR agonists published to date were limited, however, to the usage of relatively high doses given in bolus. The present study was aimed at verifying if these substances used in lower doses in combination with inhibitors of P2Y(12) could serve as components of dual anti-platelet therapy. We have found that a selective A(2A) agonist 2-hexynyl-5’-N-ethylcarboxamidoadenosine (HE-NECA) improved the anti-thrombotic properties of either cangrelor or prasugrel in the model of ferric chloride-induced experimental thrombosis in mice. Importantly, HE-NECA was effective not only when applied in bolus as other AR agonists in the up-to-date published studies, but also when given chronically. In vitro thrombus formation under flow conditions revealed that HE-NECA enhanced the ability of P2Y(12) inhibitors to decrease fibrinogen content in thrombi, possibly resulting in their lower stability. Adenosine receptor agonists possess a certain hypotensive effect and an ability to increase the blood–brain barrier permeability. Therefore, the effects of anti-thrombotic doses of HE-NECA on blood pressure and the blood–brain barrier permeability in mice were tested. HE-NECA applied in bolus caused a significant hypotension in mice, but the effect was much lower when the substance was given in doses corresponding to that obtained by chronic administration. At the same time, no significant effect of HE-NECA was observed on the blood–brain barrier. We conclude that chronic administration of the A(2A) agonist can be considered a potential component of a dual antithrombotic therapy. However, due to the hypotensive effect of the substances, dosage and administration must be elaborated to minimize the side-effects. The total number of animals used in the experiments was 146.
format Online
Article
Text
id pubmed-8002731
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-80027312021-03-28 Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus Polak, Dawid Talar, Marcin Wolska, Nina Wojkowska, Dagmara W. Karolczak, Kamil Kramkowski, Karol Bonda, Tomasz A. Watala, Cezary Przygodzki, Tomasz Int J Mol Sci Article Blood platelets’ adenosine receptors (AR) are considered to be a new target for the anti-platelet therapy. This idea is based on in vitro studies which show that signaling mediated by these receptors leads to a decreased platelet response to activating stimuli. In vivo evidence for the antithrombotic activity of AR agonists published to date were limited, however, to the usage of relatively high doses given in bolus. The present study was aimed at verifying if these substances used in lower doses in combination with inhibitors of P2Y(12) could serve as components of dual anti-platelet therapy. We have found that a selective A(2A) agonist 2-hexynyl-5’-N-ethylcarboxamidoadenosine (HE-NECA) improved the anti-thrombotic properties of either cangrelor or prasugrel in the model of ferric chloride-induced experimental thrombosis in mice. Importantly, HE-NECA was effective not only when applied in bolus as other AR agonists in the up-to-date published studies, but also when given chronically. In vitro thrombus formation under flow conditions revealed that HE-NECA enhanced the ability of P2Y(12) inhibitors to decrease fibrinogen content in thrombi, possibly resulting in their lower stability. Adenosine receptor agonists possess a certain hypotensive effect and an ability to increase the blood–brain barrier permeability. Therefore, the effects of anti-thrombotic doses of HE-NECA on blood pressure and the blood–brain barrier permeability in mice were tested. HE-NECA applied in bolus caused a significant hypotension in mice, but the effect was much lower when the substance was given in doses corresponding to that obtained by chronic administration. At the same time, no significant effect of HE-NECA was observed on the blood–brain barrier. We conclude that chronic administration of the A(2A) agonist can be considered a potential component of a dual antithrombotic therapy. However, due to the hypotensive effect of the substances, dosage and administration must be elaborated to minimize the side-effects. The total number of animals used in the experiments was 146. MDPI 2021-03-17 /pmc/articles/PMC8002731/ /pubmed/33802928 http://dx.doi.org/10.3390/ijms22063074 Text en © 2021 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Polak, Dawid
Talar, Marcin
Wolska, Nina
Wojkowska, Dagmara W.
Karolczak, Kamil
Kramkowski, Karol
Bonda, Tomasz A.
Watala, Cezary
Przygodzki, Tomasz
Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title_full Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title_fullStr Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title_full_unstemmed Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title_short Adenosine Receptor Agonist HE-NECA Enhances Antithrombotic Activities of Cangrelor and Prasugrel in vivo by Decreasing of Fibrinogen Density in Thrombus
title_sort adenosine receptor agonist he-neca enhances antithrombotic activities of cangrelor and prasugrel in vivo by decreasing of fibrinogen density in thrombus
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8002731/
https://www.ncbi.nlm.nih.gov/pubmed/33802928
http://dx.doi.org/10.3390/ijms22063074
work_keys_str_mv AT polakdawid adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT talarmarcin adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT wolskanina adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT wojkowskadagmaraw adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT karolczakkamil adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT kramkowskikarol adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT bondatomasza adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT watalacezary adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus
AT przygodzkitomasz adenosinereceptoragonisthenecaenhancesantithromboticactivitiesofcangrelorandprasugrelinvivobydecreasingoffibrinogendensityinthrombus

Ejemplares similares