EPAS1 Attenuates Atherosclerosis Initiation at Disturbed Flow Sites Through Endothelial Fatty Acid Uptake.

Pirri, Daniela; Tian, Siyu; Tardajos-Ayllon, Blanca; Irving, Sophie E; Donati, Francesco; Allen, Scott P; Mammoto, Tadanori; Vilahur, Gemma; Kabir, Lida; Bennett, Jane; Rasool, Yasmin; Pericleous, Charis; Mazzei, Guianfranco; McAllan, Liam; Scott, William R; Koestler, Thomas; Zingg, Urs; Birdsey, Graeme M; Miller, Clint L; Schenkel, Torsten; Chambers, Emily V; Dunning, Mark J; Serbanovic-Canic, Jovana; Botrè, Francesco; Mammoto, Akiko; Xu, Suowen; Osto, Elena; Han, Weiping; Fragiadaki, Maria; Evans, Paul C

Pirri, Daniela; Tian, Siyu; Tardajos-Ayllon, Blanca; Irving, Sophie E; Donati, Francesco; Allen, Scott P; Mammoto, Tadanori; Vilahur, Gemma; Kabir, Lida; Bennett, Jane; Rasool, Yasmin; Pericleous, Charis; Mazzei, Guianfranco; McAllan, Liam; Scott, William R; Koestler, Thomas; Zingg, Urs; Birdsey, Graeme M; Miller, Clint L; Schenkel, Torsten; Chambers, Emily V; Dunning, Mark J; Serbanovic-Canic, Jovana; Botrè, Francesco; Mammoto, Akiko; Xu, Suowen; Osto, Elena; Han, Weiping; Fragiadaki, Maria; Evans, Paul C.

Afiliación

Pirri D; School of Medicine and Population Health, INSIGNEO Institute, and the Bateson Centre (D.P., S.T., S.E.I., J.S.-C.), University of Sheffield, United Kingdom.
Tian S; National Heart and Lung Institute (D.P., G.M.B.), Imperial College London, United Kingdom.
Tardajos-Ayllon B; School of Medicine and Population Health, INSIGNEO Institute, and the Bateson Centre (D.P., S.T., S.E.I., J.S.-C.), University of Sheffield, United Kingdom.
Irving SE; Centre for Biochemical Pharmacology (S.T., B.T.-A., P.C.E.), William Harvey Research Institute, Barts and the London School of Medicine and Dentistry, Queen Mary University of London, United Kingdom.
Donati F; Centre for Biochemical Pharmacology (S.T., B.T.-A., P.C.E.), William Harvey Research Institute, Barts and the London School of Medicine and Dentistry, Queen Mary University of London, United Kingdom.
Allen SP; School of Medicine and Population Health, INSIGNEO Institute, and the Bateson Centre (D.P., S.T., S.E.I., J.S.-C.), University of Sheffield, United Kingdom.
Mammoto T; Laboratorio Antidoping, Federazione Medico Sportiva Italiana, Rome, Italy (F.D., F.B.).
Vilahur G; School of Medicine and Population Health, Sheffield Institute for Translational Neuroscience (S.P.A.), University of Sheffield, United Kingdom.
Kabir L; Department of Pediatrics, Department of Pharmacology and Toxicology (T.M.), Medical College of Wisconsin, Milwaukee.
Bennett J; Institut de Recerca Hospital de la Santa Creu i Sant Pau, IIB-Sant Pau, and CIBERCV (Centro de Investigación en Red de Enfermedades Cardiovasculares)-Instituto de Salud Carlos III, Barcelona, Spain (G.V.).
Rasool Y; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
Pericleous C; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
Mazzei G; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
McAllan L; Institute of Clinical Sciences, Faculty of Medicine (Y.R., G.M., L.M., W.R.S.), Imperial College London, United Kingdom.
Scott WR; Department of Surgery, Bariatric Center, Limmattal Hospital, Schlieren, Switzerland (C.P., T.K., U.Z.).
Koestler T; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
Zingg U; Institute of Clinical Sciences, Faculty of Medicine (Y.R., G.M., L.M., W.R.S.), Imperial College London, United Kingdom.
Birdsey GM; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
Miller CL; Institute of Clinical Sciences, Faculty of Medicine (Y.R., G.M., L.M., W.R.S.), Imperial College London, United Kingdom.
Schenkel T; Medical Research Council (MRC) Laboratory of Medical Sciences, London, United Kingdom (L.K., J.B., Y.R., G.M., L.M., W.R.S.).
Chambers EV; Institute of Clinical Sciences, Faculty of Medicine (Y.R., G.M., L.M., W.R.S.), Imperial College London, United Kingdom.
Dunning MJ; Department of Surgery, Bariatric Center, Limmattal Hospital, Schlieren, Switzerland (C.P., T.K., U.Z.).
Serbanovic-Canic J; Department of Surgery, Bariatric Center, Limmattal Hospital, Schlieren, Switzerland (C.P., T.K., U.Z.).
Botrè F; National Heart and Lung Institute (D.P., G.M.B.), Imperial College London, United Kingdom.
Mammoto A; Center for Public Health Genomics, Department of Public Health Sciences, University of Virginia, Charlottesville (C.L.M.).
Xu S; Department of Engineering and Mathematics, Sheffield Hallam University, United Kingdom (T.S.).
Osto E; Sheffield Bioinformatics Core, School of Medicine and Population Health (E.V.C., M.J.D.), University of Sheffield, United Kingdom.
Han W; Sheffield Bioinformatics Core, School of Medicine and Population Health (E.V.C., M.J.D.), University of Sheffield, United Kingdom.
Fragiadaki M; School of Medicine and Population Health, INSIGNEO Institute, and the Bateson Centre (D.P., S.T., S.E.I., J.S.-C.), University of Sheffield, United Kingdom.
Evans PC; Laboratorio Antidoping, Federazione Medico Sportiva Italiana, Rome, Italy (F.D., F.B.).

Circ Res ; 135(8): 822-837, 2024 Sep 27.

Article en En | MEDLINE | ID: mdl-39234692

ABSTRACT

ABSTRACT

BACKGROUND:

Atherosclerotic plaques form unevenly due to disturbed blood flow, causing localized endothelial cell (EC) dysfunction. Obesity exacerbates this process, but the underlying molecular mechanisms are unclear. The transcription factor EPAS1 (HIF2A) has regulatory roles in endothelium, but its involvement in atherosclerosis remains unexplored. This study investigates the potential interplay between EPAS1, obesity, and atherosclerosis.

METHODS:

Responses to shear stress were analyzed using cultured porcine aortic EC exposed to flow in vitro coupled with metabolic and molecular analyses and by en face immunostaining of murine aortic EC exposed to disturbed flow in vivo. Obesity and dyslipidemia were induced in mice via exposure to a high-fat diet or through Leptin gene deletion. The role of Epas1 in atherosclerosis was evaluated by inducible endothelial Epas1 deletion, followed by hypercholesterolemia induction (adeno-associated virus-PCSK9 [proprotein convertase subtilisin/kexin type 9]; high-fat diet).

RESULTS:

En face staining revealed EPAS1 enrichment at sites of disturbed blood flow that are prone to atherosclerosis initiation. Obese mice exhibited substantial reduction in endothelial EPAS1 expression. Sulforaphane, a compound with known atheroprotective effects, restored EPAS1 expression and concurrently reduced plasma triglyceride levels in obese mice. Consistently, triglyceride derivatives (free fatty acids) suppressed EPAS1 in cultured EC by upregulating the negative regulator PHD2. Clinical observations revealed that reduced serum EPAS1 correlated with increased endothelial PHD2 and PHD3 in obese individuals. Functionally, endothelial EPAS1 deletion increased lesion formation in hypercholesterolemic mice, indicating an atheroprotective function. Mechanistic insights revealed that EPAS1 protects arteries by maintaining endothelial proliferation by positively regulating the expression of the fatty acid-handling molecules CD36 (cluster of differentiation 36) and LIPG (endothelial type lipase G) to increase fatty acid beta-oxidation.

CONCLUSIONS:

Endothelial EPAS1 attenuates atherosclerosis at sites of disturbed flow by maintaining EC proliferation via fatty acid uptake and metabolism. This endothelial repair pathway is inhibited in obesity, suggesting a novel triglyceride-PHD2 modulation pathway suppressing EPAS1 expression. These findings have implications for therapeutic strategies addressing vascular dysfunction in obesity.

Asunto(s)

Aterosclerosis; Factores de Transcripción con Motivo Hélice-Asa-Hélice Básico; Células Endoteliales; Ácidos Grasos; Obesidad; Animales; Factores de Transcripción con Motivo Hélice-Asa-Hélice Básico/metabolismo; Factores de Transcripción con Motivo Hélice-Asa-Hélice Básico/genética; Aterosclerosis/metabolismo; Aterosclerosis/genética; Aterosclerosis/patología; Ratones; Células Endoteliales/metabolismo; Células Endoteliales/patología; Obesidad/metabolismo; Obesidad/genética; Células Cultivadas; Ácidos Grasos/metabolismo; Ratones Endogámicos C57BL; Porcinos; Masculino; Dieta Alta en Grasa; Endotelio Vascular/metabolismo; Endotelio Vascular/patología

Palabras clave

atherosclerosis; diet, high-fat; endothelial cells; obesity; plaque, atherosclerotic

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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Células Endoteliales / Aterosclerosis / Factores de Transcripción con Motivo Hélice-Asa-Hélice Básico / Ácidos Grasos / Obesidad Límite: Animals Idioma: En Revista: Circ Res / Circ. res / Circulation research Año: 2024 Tipo del documento: Article País de afiliación: Reino Unido Pais de publicación: Estados Unidos

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