Pharmacological inhibition of the F -ATPase/P2Y pathway suppresses the effect of apolipoprotein A1 on endothelial nitric oxide synthesis and vasorelaxation.

Cendrine Cabou,Paula Honorato,Luis Briceño,Lamia Ghezali,Thibaut Duparc,Marcelo León,Guillaume Combes,Laure Frayssinhes,Audren Fournel,Anne Abot,Bernard Masri,Nicol Parada,Valeria Aguilera,Claudio Aguayo,Claude Knauf,Marcelo González,Claudia Radojkovic,Laurent O Martinez

Acta physiologica (Oxford, England)（2019）

Cited 8|Views79

No score

Abstract

Using a pharmacological approach, we thus found that APOA1 promotes endothelial NO production and thereby controls vascular tone in a process that requires activation of the ecto-F -ATPase/P2Y pathway by APOA1. Pharmacological targeting of this pathway with respect to vascular diseases should be explored. This article is protected by copyright. All rights reserved.

Translated text

Key words

Apolipoprotein A1,F1-ATPase,endothelial cells,nitric oxide,purinergic receptors

AI Read Science

Must-Reading Tree

Example

Generate MRT to find the research sequence of this paper

Chat Paper

Summary is being generated by the instructions you defined