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Citations to this article

Regulation of acylcoenzyme A. Cholesterol acyltransferase and 3-hydroxy-3-methylglutaryl coenzyme A reductase activity by lipoproteins in the intestine of parabiont rats.
B H Purdy, F J Field
B H Purdy, F J Field
Published August 1, 1984
Citation Information: J Clin Invest. 1984;74(2):351-357. https://doi.org/10.1172/JCI111430.
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Research Article

Regulation of acylcoenzyme A. Cholesterol acyltransferase and 3-hydroxy-3-methylglutaryl coenzyme A reductase activity by lipoproteins in the intestine of parabiont rats.

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Abstract

Parabiont rats were used to study the regulation of intestinal cholesterol synthesis (3-hydroxy-3-methylglutaryl coenzyme A [HMG-CoA] reductase activity) and esterification (acylcoenzyme A/cholesterol acyltransferase [ACAT] activity) by lipoproteins and micellar cholesterol. The parabiont rat model offers a unique way to observe changes in cholesterol metabolism in the intestine, independently of luminal factors. In one group of six surgically joined pairs, one animal was fed rat chow and 0.1% propylthiouracil (PTU). Its joined mate was fed rat chow, 0.1% PTU, 5% lard, and 0.3% taurocholic acid. In another group of five pairs, one rat was fed rat chow, 0.1% PTU, 5% lard, 0.3% taurocholic acid, plus 1% cholesterol. Its joined mate was fed the same diet except the cholesterol was deleted. Serum cholesterol changes were equal between members of a given pair, attesting to their common circulation. The administration of PTU itself caused a significant elevation of serum cholesterol. When one parabiont ingested cholesterol, serum cholesterol concentrations increased significantly for both pair members compared with control pairs not ingesting cholesterol. Hepatic and intestinal HMG-CoA reductase activities were significantly decreased in rats fed the diet containing cholesterol. ACAT activities in both organs were markedly increased. This supports previous data that suggest that dietary or luminal cholesterol affects both HMG-CoA reductase and ACAT activity in the small intestine. Moreover, in rats that were hypercholesterolemic but not ingesting dietary cholesterol, hepatic and intestinal reductase activities were decreased and ACAT activities were increased compared with the control animals. Intestinal microsomal cholesterol content was increased only in rats fed cholesterol. No changes in intestinal microsomal cholesterol were observed in the other animals. The data suggest that intestinal HMG-CoA reductase and ACAT activities are regulated by plasma lipoproteins independently of luminal factors. This nonluminal regulatory effect occurs without a measurable contribution to the intestinal microsomal cholesterol pool.

Authors

B H Purdy, F J Field

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Total citations by year

Year: 2021 2009 2002 2001 1999 1998 1994 1993 1990 1988 1987 1986 1985 Total
Citations: 1 1 2 2 1 1 1 1 1 2 2 2 2 19
Citation information
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Citations to this article (19)

Title and authors Publication Year
Yeast β-glucan reduces obesity-associated Bilophila abundance and modulates bile acid metabolism in healthy and high-fat diet mouse models
SY So, Q Wu, KS Leung, ZM Kundi, TC Savidge, H El-Nezami
AJP Gastrointestinal and Liver Physiology 2021
Lipoproteins, cholesterol homeostasis and cardiac health
TF Daniels, KM Killinger, JJ Michal, RW Wright, Z Jiang
International journal of biological sciences 2009
Up-regulation of acyl-coenzyme A:cholesterol acyltransferase (ACAT) in nephrotic syndrome
ND Vaziri, K Liang
Kidney International 2002
Upregulation of acyl-CoA:cholesterol acyltransferase in chronic renal failure
K Liang, ND Vaziri
American journal of physiology. Endocrinology and metabolism 2002
Intestinal Lipid Metabolism
CM Mansbach, P Tso, A Kuksis
2001
Mechanisms for cholesterol homeostasis in rat jejunal mucosa: effects of cholesterol, sitosterol, and lovastatin
LB Nguyen, S Shefer, G Salen, GS Tint, F Ruiz, J Bullock
Journal of lipid research 2001
Intestinal cholesterol absorption
PA Dawson, LL Rudel
Current Opinion in Lipidology 1999
Identification of a Form of Acyl-CoA:Cholesterol Acyltransferase Specific to Liver and Intestine in Nonhuman Primates
RA Anderson, C Joyce, M Davis, JW Reagan, M Clark, GS Shelness, LL Rudel
The Journal of biological chemistry 1998
Deficient ileal 3-hydroxy-3-methylglutaryl coenzyme A reductase activity in sitosterolemia: Sitosterol is not a feedback inhibitor of intestinal cholesterol biosynthesis
LB Nguyen, G Salen, S Shefer, J Bullock, T Chen, GS Tint, IR Chowdhary, S Lerner
Metabolism 1994
Regulation of LDL receptor expression by luminal sterol flux in CaCo-2 cells
FJ Field, D Fujiwara, E Born, DA Chappell, SN Mathur
Arteriosclerosis Thrombosis and Vascular Biology 1993
Regulation of cholesterol metabolism in the intestine
FJ Field, NT Kam, SN Mathur
Gastroenterology 1990
Intestinal HMG-CoA reductase activity is low in hypercholesterolemic patients and is further decreased with lovastatin therapy
ML Freeman, WF Prigge, DB Hunninghake, WC Duane, RL Gebhard
Journal of lipid research 1988
Modification of CaCo-2 cell membrane fatty acid composition by eicosapentaenoic acid and palmitic acid: effect on cholesterol metabolism
S Murthy, E Albright, SN Mathur, FJ Field
Journal of lipid research 1988
Intestinal apolipoprotein A-I and B-48 metabolism: effects of sustained alterations in dietary triglyceride and mucosal cholesterol flux
NO Davidson, AM Magun, TA Brasitus, RM Glickman
Journal of lipid research 1987
Regulation of cholesterol esterification by micellar cholesterol in CaCo-2 cells
FJ Field, E Albright, SN Mathur
Journal of lipid research 1987
The effect of hypothyroidism and thyroxine replacement on hepatic and intestinal HMG-CoA reductase and ACAT activities and biliary lipids in the rat
FJ Field, E Albright, SN Mathur
Metabolism 1986
Effect of dietary cholesterol on biliary cholesterol content and bile flow in the hypothyroid rat
FJ Field, E Albright, SN Mathur
Gastroenterology 1986
Regulation of Hmg-coa Reductase
LC Smith, AM Gotto
Regulation of Hmg-coa Reductase 1985
Role of acyl-CoA: cholesterol acyltransferase in cellular cholesterol metabolism
KE Suckling, EF Stange
Journal of lipid research 1985

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