Atorvastatin protects obese mice against hepatic ischemia-reperfusion injury by Toll-like receptor-4 suppression and endothelial nitric oxide synthase activation

dc.contributor.authorAjamieh, Hussam
dc.contributor.authorFarrell, Geoffrey
dc.contributor.authorWong, Heng
dc.contributor.authorYu, Jun
dc.contributor.authorChu, Eagle
dc.contributor.authorChen, Jeffrey
dc.contributor.authorTeoh, Narcissus
dc.date.accessioned2015-12-10T23:17:54Z
dc.date.issued2012
dc.date.updated2016-02-24T08:37:40Z
dc.description.abstractBackground and Aim: Steatosis accentuates the severity of hepatic ischemia-reperfusion injury (IRI). 3-Hydroxy-3-methylglutaryl-coenzyme A reductase inhibitors ("statins") protect the heart and brain against post-ischemic injury, without necessarily lowering serum cholesterol. We tested whether 10-day or 1-day atorvastatin administration protects livers with fatty change or non-alcoholic steatohepatitis (NASH) against IRI. Methods: Mice with dietary or genetic simple steatosis (SS) or NASH were subjected to 60min of partial hepatic ischemia/24-h reperfusion, with/without atorvastatin administered with food (5mg/kg body weight) for 10days, or injected intravenously (5mg/kg) 24h before ischemia. Liver injury, Toll-like receptor-4 (TLR4), cytokines/chemokines, endothelial nitric oxide synthase (eNOS), activation and thromboxane B2 production were determined. Results: Atorvastatin conferred 70-90% hepatic protection against IRI in obese animals with SS or NASH, in which IRI was accentuated twofold to fivefold. IRI markedly upregulated TLR4 and activated nuclear factor-κB (NF-κB); atorvastatin abrogated these effects, as well as activating eNOS. Atorvastatin dampened the post-ischemic induction of thromboxane B2, macrophage inflammatory protein-1a, monocyte chemotactic protein-1, tumor necrosis factor-α, interleukin (IL)-12 p40, γ-interferon, IL-6, and adhesion molecules (vascular cell adhesion molecule-1, E-selectin, vascular endothelial-cadherin), and reduced macrophage and neutrophil recruitment. There was no reduction in serum cholesterol that could explain these effects, and hepatic cholesterol was normal in these mice. A single 24-h injection of atorvastatin conferred equivalent hepatoprotection. Conclusion: Statins exert major hepatoprotection against IRI in lean, fatty, and NASH livers that is not due to cholesterol removal. Rather, statins downregulate TLR4 to prevent NF-κB activation, with resultant suppression of adhesion molecules, chemokines/cytokines, and thromboxane B2 production. Short-term statin treatment is an effective, readily-available preventive agent against hepatic IRI, irrespective of obesity and fatty liver disease.
dc.identifier.issn0815-9319
dc.identifier.urihttp://hdl.handle.net/1885/65394
dc.publisherBlackwell Publishing Ltd
dc.sourceJournal of Gastroenterology and Hepatology
dc.subjectKeywords: alanine aminotransferase; atorvastatin; cholesterol; endothelial leukocyte adhesion molecule 1; endothelial nitric oxide synthase; gamma interferon; I kappa B alpha; immunoglobulin enhancer binding protein; interleukin 12p40; macrophage inflammatory prote Atorvastatin; Liver inflammation; Non-alcoholic fatty liver disease; Nuclear factor-?B; Toll-like receptor-4
dc.titleAtorvastatin protects obese mice against hepatic ischemia-reperfusion injury by Toll-like receptor-4 suppression and endothelial nitric oxide synthase activation
dc.typeJournal article
local.bibliographicCitation.issue8
local.bibliographicCitation.lastpage1361
local.bibliographicCitation.startpage1353
local.contributor.affiliationAjamieh, Hussam, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationFarrell, Geoffrey, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationWong, Heng, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationYu, Jun, Li KaShing Institute of Health Sciences
local.contributor.affiliationChu, Eagle, Li KaShing Institute of Health Sciences
local.contributor.affiliationChen, Jeffrey, College of Medicine, Biology and Environment, ANU
local.contributor.affiliationTeoh, Narcissus, College of Medicine, Biology and Environment, ANU
local.contributor.authoremailu4028700@anu.edu.au
local.contributor.authoruidAjamieh, Hussam, u4715759
local.contributor.authoruidFarrell, Geoffrey, u4028700
local.contributor.authoruidWong, Heng, u4090977
local.contributor.authoruidChen, Jeffrey, u4787026
local.contributor.authoruidTeoh, Narcissus, u4325419
local.description.embargo2037-12-31
local.description.notesImported from ARIES
local.identifier.absfor110300 - CLINICAL SCIENCES
local.identifier.ariespublicationf5625xPUB1099
local.identifier.citationvolume27
local.identifier.doi10.1111/j.1440-1746.2012.07123.x
local.identifier.scopusID2-s2.0-84864302073
local.identifier.thomsonID000306650700017
local.identifier.uidSubmittedByf5625
local.type.statusPublished Version

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