Atorvastatin protects obese mice against hepatic ischemia-reperfusion injury by Toll-like receptor-4 suppression and endothelial nitric oxide synthase activation
dc.contributor.author | Ajamieh, Hussam | |
dc.contributor.author | Farrell, Geoffrey | |
dc.contributor.author | Wong, Heng | |
dc.contributor.author | Yu, Jun | |
dc.contributor.author | Chu, Eagle | |
dc.contributor.author | Chen, Jeffrey | |
dc.contributor.author | Teoh, Narcissus | |
dc.date.accessioned | 2015-12-10T23:17:54Z | |
dc.date.issued | 2012 | |
dc.date.updated | 2016-02-24T08:37:40Z | |
dc.description.abstract | Background 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.issn | 0815-9319 | |
dc.identifier.uri | http://hdl.handle.net/1885/65394 | |
dc.publisher | Blackwell Publishing Ltd | |
dc.source | Journal of Gastroenterology and Hepatology | |
dc.subject | Keywords: 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.title | Atorvastatin protects obese mice against hepatic ischemia-reperfusion injury by Toll-like receptor-4 suppression and endothelial nitric oxide synthase activation | |
dc.type | Journal article | |
local.bibliographicCitation.issue | 8 | |
local.bibliographicCitation.lastpage | 1361 | |
local.bibliographicCitation.startpage | 1353 | |
local.contributor.affiliation | Ajamieh, Hussam, College of Medicine, Biology and Environment, ANU | |
local.contributor.affiliation | Farrell, Geoffrey, College of Medicine, Biology and Environment, ANU | |
local.contributor.affiliation | Wong, Heng, College of Medicine, Biology and Environment, ANU | |
local.contributor.affiliation | Yu, Jun, Li KaShing Institute of Health Sciences | |
local.contributor.affiliation | Chu, Eagle, Li KaShing Institute of Health Sciences | |
local.contributor.affiliation | Chen, Jeffrey, College of Medicine, Biology and Environment, ANU | |
local.contributor.affiliation | Teoh, Narcissus, College of Medicine, Biology and Environment, ANU | |
local.contributor.authoremail | u4028700@anu.edu.au | |
local.contributor.authoruid | Ajamieh, Hussam, u4715759 | |
local.contributor.authoruid | Farrell, Geoffrey, u4028700 | |
local.contributor.authoruid | Wong, Heng, u4090977 | |
local.contributor.authoruid | Chen, Jeffrey, u4787026 | |
local.contributor.authoruid | Teoh, Narcissus, u4325419 | |
local.description.embargo | 2037-12-31 | |
local.description.notes | Imported from ARIES | |
local.identifier.absfor | 110300 - CLINICAL SCIENCES | |
local.identifier.ariespublication | f5625xPUB1099 | |
local.identifier.citationvolume | 27 | |
local.identifier.doi | 10.1111/j.1440-1746.2012.07123.x | |
local.identifier.scopusID | 2-s2.0-84864302073 | |
local.identifier.thomsonID | 000306650700017 | |
local.identifier.uidSubmittedBy | f5625 | |
local.type.status | Published Version |
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