Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]

Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]

Obesity-associated chronic inflammation contributes to metabolic dysfunction and propagates atherosclerosis. Recent evidence suggests that increased dietary cholesterol exacerbates inflammation in adipose tissue and liver, contributing to the proatherogenic milieu. The ability of the citrus flavonoi...

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Main Authors: Julia M. Assini, Erin E. Mulvihill, Brian G. Sutherland, Dawn E. Telford, Cynthia G. Sawyez, Sarah L. Felder, Sanjiv Chhoker, Jane Y. Edwards, Robert Gros, Murray W. Huff
Format: Article
Language:English
Published: Elsevier 2013-03-01
Series:Journal of Lipid Research
Subjects:
cholesterol
flavonoid
lipids
obesity
hepatic steatosis
insulin resistance
Online Access:http://www.sciencedirect.com/science/article/pii/S0022227520419352
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spelling doaj-158247674e644e5aa756021704b6e7ce2021-04-28T06:05:37ZengElsevierJournal of Lipid Research0022-22752013-03-01543711724Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]Julia M. Assini0Erin E. Mulvihill1Brian G. Sutherland2Dawn E. Telford3Cynthia G. Sawyez4Sarah L. Felder5Sanjiv Chhoker6Jane Y. Edwards7Robert Gros8Murray W. Huff9Vascular Biology, Robarts Research Institute; Department of BiochemistryVascular Biology, Robarts Research Institute; Department of BiochemistryVascular Biology, Robarts Research InstituteVascular Biology, Robarts Research Institute; Department of MedicineVascular Biology, Robarts Research Institute; Department of MedicineVascular Biology, Robarts Research Institute; Department of BiochemistryVascular Biology, Robarts Research Institute; Department of BiochemistryVascular Biology, Robarts Research Institute; Department of MedicineVascular Biology, Robarts Research Institute; Department of Medicine; Department of Physiology and Pharmacology, University of Western Ontario, London, Ontario, CanadaTo whom correspondence should be addressed. e-mail: mhuff@uwo.ca.; Vascular Biology, Robarts Research Institute; Department of Biochemistry; Department of MedicineObesity-associated chronic inflammation contributes to metabolic dysfunction and propagates atherosclerosis. Recent evidence suggests that increased dietary cholesterol exacerbates inflammation in adipose tissue and liver, contributing to the proatherogenic milieu. The ability of the citrus flavonoid naringenin to prevent these cholesterol-induced perturbations is unknown. To assess the ability of naringenin to prevent the amplified inflammatory response and atherosclerosis induced by dietary cholesterol, male Ldlr−/− mice were fed either a cholesterol-enriched high-fat or low-fat diet supplemented with 3% naringenin for 12 weeks. Naringenin, through induction of hepatic fatty acid (FA) oxidation and attenuation of FA synthesis, prevented hepatic steatosis, hepatic VLDL overproduction, and hyperlipidemia induced by both cholesterol-rich diets. Naringenin attenuated hepatic macrophage infiltration and inflammation stimulated by dietary cholesterol. Insulin resistance, adipose tissue expansion, and inflammation were alleviated by naringenin. Naringenin attenuated the cholesterol-induced formation of both foam cells and expression of inflammatory markers in peritoneal macrophages. Naringenin significantly decreased atherosclerosis and inhibited the formation of complex lesions, which was associated with normalized aortic lipids and a reversal of aortic inflammation. We demonstrate that in mice fed cholesterol-enriched diets, naringenin attenuates peripheral and systemic inflammation, leading to protection from atherosclerosis. These studies offer a therapeutically relevant alternative for the prevention of cholesterol-induced metabolic dysregulation.http://www.sciencedirect.com/science/article/pii/S0022227520419352cholesterolflavonoidlipidsobesityhepatic steatosisinsulin resistance
collection DOAJ
language English
format Article
sources DOAJ
author Julia M. Assini
Erin E. Mulvihill
Brian G. Sutherland
Dawn E. Telford
Cynthia G. Sawyez
Sarah L. Felder
Sanjiv Chhoker
Jane Y. Edwards
Robert Gros
Murray W. Huff
spellingShingle Julia M. Assini
Erin E. Mulvihill
Brian G. Sutherland
Dawn E. Telford
Cynthia G. Sawyez
Sarah L. Felder
Sanjiv Chhoker
Jane Y. Edwards
Robert Gros
Murray W. Huff
Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
Journal of Lipid Research
cholesterol
flavonoid
lipids
obesity
hepatic steatosis
insulin resistance
author_facet Julia M. Assini
Erin E. Mulvihill
Brian G. Sutherland
Dawn E. Telford
Cynthia G. Sawyez
Sarah L. Felder
Sanjiv Chhoker
Jane Y. Edwards
Robert Gros
Murray W. Huff
author_sort Julia M. Assini
title Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
title_short Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
title_full Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
title_fullStr Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
title_full_unstemmed Naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in Ldlr−/− mice[S]
title_sort naringenin prevents cholesterol-induced systemic inflammation, metabolic dysregulation, and atherosclerosis in ldlr−/− mice[s]
publisher Elsevier
series Journal of Lipid Research
issn 0022-2275
publishDate 2013-03-01
description Obesity-associated chronic inflammation contributes to metabolic dysfunction and propagates atherosclerosis. Recent evidence suggests that increased dietary cholesterol exacerbates inflammation in adipose tissue and liver, contributing to the proatherogenic milieu. The ability of the citrus flavonoid naringenin to prevent these cholesterol-induced perturbations is unknown. To assess the ability of naringenin to prevent the amplified inflammatory response and atherosclerosis induced by dietary cholesterol, male Ldlr−/− mice were fed either a cholesterol-enriched high-fat or low-fat diet supplemented with 3% naringenin for 12 weeks. Naringenin, through induction of hepatic fatty acid (FA) oxidation and attenuation of FA synthesis, prevented hepatic steatosis, hepatic VLDL overproduction, and hyperlipidemia induced by both cholesterol-rich diets. Naringenin attenuated hepatic macrophage infiltration and inflammation stimulated by dietary cholesterol. Insulin resistance, adipose tissue expansion, and inflammation were alleviated by naringenin. Naringenin attenuated the cholesterol-induced formation of both foam cells and expression of inflammatory markers in peritoneal macrophages. Naringenin significantly decreased atherosclerosis and inhibited the formation of complex lesions, which was associated with normalized aortic lipids and a reversal of aortic inflammation. We demonstrate that in mice fed cholesterol-enriched diets, naringenin attenuates peripheral and systemic inflammation, leading to protection from atherosclerosis. These studies offer a therapeutically relevant alternative for the prevention of cholesterol-induced metabolic dysregulation.
topic cholesterol
flavonoid
lipids
obesity
hepatic steatosis
insulin resistance
url http://www.sciencedirect.com/science/article/pii/S0022227520419352
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