Combined sub-optimal doses of Rosuvastatin and Bexarotene impairs angiotensin II-induced arterial mononuclear cell adhesion through inhibition of Nox5 signaling pathways and increased RXR/PPARα and RXR/PPARγ interactions

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RESEARCH PRODUCT

Combined sub-optimal doses of Rosuvastatin and Bexarotene impairs angiotensin II-induced arterial mononuclear cell adhesion through inhibition of Nox5 signaling pathways and increased RXR/PPARα and RXR/PPARγ interactions

Gonzalez-navarroherminia Sanzmaria-jesus Hermenegildocarlos Piqueraslaura Escuderopaula Peiróconcepción Martinez De Marañónaranzazu Colladoaida

subject

medicine.medical_specialty Tetrahydronaphthalenes Physiology Peroxisome Proliferator-Activated Receptors Clinical Biochemistry CCL2 Biology Nitric Oxide Biochemistry Peripheral blood mononuclear cell Cell Line Internal medicine Cell Adhesion medicine Anticarcinogenic Agents Humans Rosuvastatin Interleukin 8 Rosuvastatin Calcium Molecular Biology General Environmental Science Sistema cardiovascular Bexarotene Sulfonamides Diabetis Artèries Angiotensin II Membrane Proteins NADPH Oxidases Arteries Cell Biology Angiotensin II Fluorobenzenes CXCL1 Original Research Communications Pyrimidines Retinoid X Receptors Endocrinology NADPH Oxidase 5 Bexarotene Leukocytes Mononuclear General Earth and Planetary Sciences Signal transduction Signal Transduction medicine.drug

description

Aim: Mononuclear cell (MC) infiltration into the arterial subendothelium is a key event in atherogenesis. Rosuvastatin (Rosu) and bexarotene (Bex) exert anti-inflammatory activity, but serious dose-related adverse effects have emerged. The need for safer and effective strategies to prevent and treat atherosclerosis led us to test the effect of combined use of both drugs on angiotensin II (Ang-II)-induced arterial MC recruitment. Results: Vehicle, Rosu (10–30 nM), Bex (0.3–1 μM), or a combination of both were administered to human umbilical arterial endothelial cells (HUAECs) 20 h before stimulation with 1 μM Ang-II (4 h). Surprisingly, a combination of Rosu (10 nM)+Bex (0.3 μM), which did not influence Ang-II-induced MC recruitment when either stimulus was studied alone, significantly reduced this response. This effect was accompanied by diminished Ang-II-induced ICAM-1, VCAM-1, and CX3CL1 endothelial expression and CXCL1, CXCL8, CCL2, and CCL5 production. Preincubation of HUAECs with Rosu+Bex inhibited Nox5 expression and Nox5-induced RhoA activation stimulated by Ang-II through increased RXRα, PPARα, and PPARγ expression in addition to RXRα/PPARα and RXRα/PPARγ interactions. In vivo, combined but not single administration of Rosu (1.25 mg/kg/day) and Bex (10 mg/kg/day) significantly diminished Ang-II-induced arteriolar leukocyte adhesion in the cremasteric microcirculation of C57BL/6 mice and atherosclerotic lesion formation in apoE−/− mice subjected to an atherogenic diet. Innovation and Conclusion: Combined administration of Bex+Rosu at suboptimal doses may constitute a new alternative and effective therapy in the control of the vascular inflammation associated to cardiometabolic disorders, since they synergize in their anti-inflammatory actions and may counteract their associated adverse effects. Antioxid. Redox Signal. 22, 901–920.

year	journal	country	edition	language
2015-04-10

10.1089/ars.2014.5969 https://hdl.handle.net/10550/75710