Literature DB >> 2930479

Processing of cholesteryl ester from low-density lipoproteins in the rat. Hepatic metabolism and biliary secretion after uptake by different hepatic cell types.

F Kuipers1, J F Nagelkerke, H Bakkeren, R Havinga, T J Van Berkel, R J Vonk.   

Abstract

Biliary secretion of the cholesteryl ester moiety of (modified) low-density lipoprotein (LDL) was examined under various experimental conditions in the rat. Human LDL or acetylated LDL (acetyl-LDL), radiolabelled with [3H]cholesteryl oleate, was administered intravenously to unanesthetized rats equipped with permanent catheters in the bile duct, duodenum and heart. LDL was cleared relatively slowly from plasma, mainly by Kupffer cells. At 3 h after injection, only 0.9% of the radioactivity was found in bile; after 12 h this value was 4.5%. Uptake of LDL by hepatocytes was stimulated by treatment of the rats with 17 alpha-ethinyloestradiol (EE; 5 mg/kg for 3 successive days); this resulted in a more rapid secretion of radioactivity into bile, 3.9% and 12.4% after 3 h and 12 h respectively. The extremely rapid uptake of acetyl-LDL via the scavenger pathway, mainly by endothelial cells, resulted in the secretion of only 2.1% of its 3H label into bile within 3 h, and 9.5% within 12 h. Radioactivity in bile was predominantly in the form of bile acids; only a small part was secreted as free cholesterol. However, the specific radioactivity of biliary cholesterol was higher than that of bile acids in all three experimental conditions. EE-treated animals did not form cholic acid from [3H]cholesteryl oleate, which was a major product of the cholesteryl oleate from LDL and acetyl-LDL in untreated rats, but formed predominantly very polar bile acids, i.e. muricholic acids. It is concluded that uptake of human LDL or acetyl-LDL by the liver of untreated rats is not efficiently coupled to biliary secretion of cholesterol (bile acids). This might be due to the anatomical localization of their principal uptake sites, the Kupffer cells and the endothelial cells respectively. Induction of LDL uptake by hepatocytes by EE treatment warrants a more efficient disposition of cholesterol from the body via bile.

Entities:  

Mesh:

Substances:

Year:  1989        PMID: 2930479      PMCID: PMC1135644          DOI: 10.1042/bj2570699

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  30 in total

1.  Degradation of cationized low density lipoprotein and regulation of cholesterol metabolism in homozygous familial hypercholesterolemia fibroblasts.

Authors:  S K Basu; J L Goldstein; G W Anderson; M S Brown
Journal:  Proc Natl Acad Sci U S A       Date:  1976-09       Impact factor: 11.205

2.  Effect of ethynylestradiol on biliary excretion of bile acids, phosphatidylcolines, and cholesterol in the bile fistula rat.

Authors:  F Kern; H Eriksson; T Curstedt; J Sjövall
Journal:  J Lipid Res       Date:  1977-09       Impact factor: 5.922

3.  Mechanism of estrogen-induced saturated bile in the hamster.

Authors:  G G Bonorris; M J Coyne; A Chung; L J Schoenfield
Journal:  J Lab Clin Med       Date:  1977-12

4.  The activity of an esterified cholesterol transferring factor in human and rat serum.

Authors:  P J Barter; J I Lally
Journal:  Biochim Biophys Acta       Date:  1978-11-22

5.  The plasma volume of the Wistar rat in relation to the body weight.

Authors:  M K Bijsterbosch; A M Duursma; J M Bouma; M Gruber
Journal:  Experientia       Date:  1981-04-15

6.  Hepatic catabolism of rat and human lipoproteins in rats treated with 17 alpha-ethinyl estradiol.

Authors:  Y S Chao; E E Windler; G C Chen; R J Havel
Journal:  J Biol Chem       Date:  1979-11-25       Impact factor: 5.157

7.  Bile secretion and bile composition in the freely moving, unanaesthetized rat with a permanent biliary drainage: influence of food intake on bile flow.

Authors:  R J Vonk; A B van Doorn; J H Strubbe
Journal:  Clin Sci Mol Med       Date:  1978-09

8.  Reversal by triton WR-1339 of ethynyloestradiol-induced hepatic cholesterol esterification.

Authors:  R A Davis; R Showalter; F Kern
Journal:  Biochem J       Date:  1978-07-15       Impact factor: 3.857

9.  Quantification of LDL cholesteryl ester contribution to biliary steroids in the rat.

Authors:  S Bhattacharya; S Balasubramaniam; L A Simons
Journal:  Biochim Biophys Acta       Date:  1986-05-21

10.  Hepatic processing of the cholesteryl ester from low density lipoprotein in the rat.

Authors:  J F Nagelkerke; H F Bakkeren; F Kuipers; R J Vonk; T J van Berkel
Journal:  J Biol Chem       Date:  1986-07-05       Impact factor: 5.157
View more
  4 in total

1.  Evidence for reverse cholesterol transport in vivo from liver endothelial cells to parenchymal cells and bile by high-density lipoprotein.

Authors:  H F Bakkeren; F Kuipers; R J Vonk; T J Van Berkel
Journal:  Biochem J       Date:  1990-06-15       Impact factor: 3.857

2.  Short- and long-term effects of biliary drainage on hepatic cholesterol metabolism in the rat.

Authors:  M J Smit; A M Temmerman; R Havinga; F Kuipers; R J Vonk
Journal:  Biochem J       Date:  1990-08-01       Impact factor: 3.857

3.  High density lipoproteins, but not other lipoproteins, provide a vehicle for sterol transport to bile.

Authors:  S J Robins; J M Fasulo
Journal:  J Clin Invest       Date:  1997-02-01       Impact factor: 14.808

4.  Selective uptake of cholesteryl esters from apolipoprotein-E-free high-density lipoproteins by rat parenchymal cells in vivo is efficiently coupled to bile acid synthesis.

Authors:  M N Pieters; D Schouten; H F Bakkeren; B Esbach; A Brouwer; D L Knook; T J van Berkel
Journal:  Biochem J       Date:  1991-12-01       Impact factor: 3.857
  4 in total

北京卡尤迪生物科技股份有限公司 © 2022-2023.