Literature DB >> 18340009

Cholesterol synthesis inhibition elicits an integrated molecular response in human livers including decreased ACAT2.

Paolo Parini1, Ulf Gustafsson, Matt A Davis, Lilian Larsson, Curt Einarsson, Martha Wilson, Mats Rudling, Hiroshi Tomoda, Satoshi Omura, Staffan Sahlin, Bo Angelin, Lawrence L Rudel, Mats Eriksson.   

Abstract

OBJECTIVE: The purpose of this study was to identify how different degrees of cholesterol synthesis inhibition affect human hepatic cholesterol metabolism. METHODS AND
RESULTS: Thirty-seven normocholesterolemic gallstone patients randomized to treatment with placebo, 20 mg/d fluvastatin, or 80 mg/d atorvastatin for 4 weeks were studied. Based on serum lathosterol determinations, cholesterol synthesis was reduced by 42% and 70% in the 2 groups receiving statins. VLDL cholesterol was reduced by 20% and 55%. During gallstone surgery, a liver biopsy was obtained and hepatic protein and mRNA expression of rate-limiting steps in cholesterol metabolism were assayed and related to serum lipoproteins. A marked induction of LDL receptors and 3-hydroxy-3-methylglutaryl (HMG) coenzyme A (CoA) reductase was positively related to the degree of cholesterol synthesis inhibition (ChSI). The activity, protein, and mRNA for ACAT2 were all reduced during ChSI, as was apoE mRNA. The lowering of HDL cholesterol in response to high ChSI could not be explained by altered expression of the HDL receptor CLA-1, ABCA1, or apoA-I.
CONCLUSIONS: Statin treatment reduces ACAT2 activity in human liver and this effect, in combination with a reduced Apo E expression, may contribute to the favorable lowering of VLDL cholesterol seen in addition to the LDL lowering during statin treatment.

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Year:  2008        PMID: 18340009      PMCID: PMC2757773          DOI: 10.1161/ATVBAHA.107.157172

Source DB:  PubMed          Journal:  Arterioscler Thromb Vasc Biol        ISSN: 1079-5642            Impact factor:   8.311


  25 in total

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Authors:  Camilla Pramfalk; Matthew A Davis; Mats Eriksson; Lawrence L Rudel; Paolo Parini
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2.  Lipoprotein profiles in plasma and interstitial fluid analyzed with an automated gel-filtration system.

Authors:  P Parini; L Johansson; A Bröijersén; B Angelin; M Rudling
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Review 5.  Acyl coenzyme A: cholesterol acyltransferase types 1 and 2: structure and function in atherosclerosis.

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7.  Biliary lipid composition in patients with cholesterol and pigment gallstones and gallstone-free subjects: deoxycholic acid does not contribute to formation of cholesterol gallstones.

Authors:  U Gustafsson; S Sahlin; C Einarsson
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9.  Bile acids and lipoprotein metabolism: effects of cholestyramine and chenodeoxycholic acid on human hepatic mRNA expression.

Authors:  L-M Nilsson; A Abrahamsson; S Sahlin; U Gustafsson; B Angelin; P Parini; C Einarsson
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10.  Overexpression and accumulation of apolipoprotein E as a cause of hypertriglyceridemia.

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2.  Effect of atorvastatin on testosterone levels.

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4.  Ezetimibe in Combination With Simvastatin Reduces Remnant Cholesterol Without Affecting Biliary Lipid Concentrations in Gallstone Patients.

Authors:  Osman Ahmed; Karin Littmann; Ulf Gustafsson; Camilla Pramfalk; Katariina Öörni; Lilian Larsson; Mirko E Minniti; Staffan Sahlin; German Camejo; Paolo Parini; Mats Eriksson
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5.  The "Mevalonate hypothesis": a cholesterol-independent alternative for the etiology of atherosclerosis.

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