Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains

Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains

Although lipid-rich microdomains of hepatocyte plasma membranes serve as the major scaffolding regions for cholesterol transport proteins important in cholesterol disposition, little is known regarding intracellular factors regulating cholesterol distribution therein. On the basis of its ability to...

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Main Authors: Avery L. McIntosh, Barbara P. Atshaves, Stephen M. Storey, Kerstin K. Landrock, Danilo Landrock, Gregory G. Martin, Ann B. Kier, Friedhelm Schroeder
Format: Article
Language:English
Published: Elsevier 2012-03-01
Series:Journal of Lipid Research
Subjects:
fatty acid
cholesterol
high density lipoprotein
lipids
liver
membranes
Online Access:http://www.sciencedirect.com/science/article/pii/S0022227520413628
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spelling doaj-eb28740efce2411a8700e8aed2e6ee3f2021-04-28T06:04:39ZengElsevierJournal of Lipid Research0022-22752012-03-01533467480Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomainsAvery L. McIntosh0Barbara P. Atshaves1Stephen M. Storey2Kerstin K. Landrock3Danilo Landrock4Gregory G. Martin5Ann B. Kier6Friedhelm Schroeder7Department of Physiology and Pharmacology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andDepartment of Biochemistry & Molecular Biology, Michigan State University, East Lansing, MI 48824Department of Physiology and Pharmacology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andDepartment of Physiology and Pharmacology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andDepartment of Pathobiology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andDepartment of Physiology and Pharmacology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andDepartment of Pathobiology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andTo whom correspondence should be addressed; Department of Physiology and Pharmacology, Texas A&M University Texas Veterinary Medical Center, College Station, TX 77843; andAlthough lipid-rich microdomains of hepatocyte plasma membranes serve as the major scaffolding regions for cholesterol transport proteins important in cholesterol disposition, little is known regarding intracellular factors regulating cholesterol distribution therein. On the basis of its ability to bind cholesterol and alter hepatic cholesterol accumulation, the cytosolic liver type FA binding protein (L-FABP) was hypothesized to be a candidate protein regulating these microdomains. Compared with wild-type hepatocyte plasma membranes, L-FABP gene ablation significantly increased the proportion of cholesterol-rich microdomains. Lack of L-FABP selectively increased cholesterol, phospholipid (especially phosphatidylcholine), and branched-chain FA accumulation in the cholesterol-rich microdomains. These cholesterol-rich microdomains are important, owing to enrichment therein of significant amounts of key transport proteins involved in uptake of cholesterol [SR-B1, ABCA-1, P-glycoprotein (P-gp), sterol carrier binding protein (SCP-2)], FA transport protein (FATP), and glucose transporters 1 and 2 (GLUT1, GLUT2) insulin receptor. L-FABP gene ablation enhanced the concentration of SCP-2, SR-B1, FATP4, and GLUT1 in the cholesterol-poor microdomains, with functional implications in HDL-mediated uptake and efflux of cholesterol. Thus L-FABP gene ablation significantly impacted the proportion of cholesterol-rich versus -poor microdomains in the hepatocyte plasma membrane and altered the distribution of lipids and proteins involved in cholesterol uptake therein.http://www.sciencedirect.com/science/article/pii/S0022227520413628fatty acidcholesterolhigh density lipoproteinlipidslivermembranes
collection DOAJ
language English
format Article
sources DOAJ
author Avery L. McIntosh
Barbara P. Atshaves
Stephen M. Storey
Kerstin K. Landrock
Danilo Landrock
Gregory G. Martin
Ann B. Kier
Friedhelm Schroeder
spellingShingle Avery L. McIntosh
Barbara P. Atshaves
Stephen M. Storey
Kerstin K. Landrock
Danilo Landrock
Gregory G. Martin
Ann B. Kier
Friedhelm Schroeder
Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
Journal of Lipid Research
fatty acid
cholesterol
high density lipoprotein
lipids
liver
membranes
author_facet Avery L. McIntosh
Barbara P. Atshaves
Stephen M. Storey
Kerstin K. Landrock
Danilo Landrock
Gregory G. Martin
Ann B. Kier
Friedhelm Schroeder
author_sort Avery L. McIntosh
title Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
title_short Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
title_full Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
title_fullStr Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
title_full_unstemmed Loss of liver FA binding protein significantly alters hepatocyte plasma membrane microdomains
title_sort loss of liver fa binding protein significantly alters hepatocyte plasma membrane microdomains
publisher Elsevier
series Journal of Lipid Research
issn 0022-2275
publishDate 2012-03-01
description Although lipid-rich microdomains of hepatocyte plasma membranes serve as the major scaffolding regions for cholesterol transport proteins important in cholesterol disposition, little is known regarding intracellular factors regulating cholesterol distribution therein. On the basis of its ability to bind cholesterol and alter hepatic cholesterol accumulation, the cytosolic liver type FA binding protein (L-FABP) was hypothesized to be a candidate protein regulating these microdomains. Compared with wild-type hepatocyte plasma membranes, L-FABP gene ablation significantly increased the proportion of cholesterol-rich microdomains. Lack of L-FABP selectively increased cholesterol, phospholipid (especially phosphatidylcholine), and branched-chain FA accumulation in the cholesterol-rich microdomains. These cholesterol-rich microdomains are important, owing to enrichment therein of significant amounts of key transport proteins involved in uptake of cholesterol [SR-B1, ABCA-1, P-glycoprotein (P-gp), sterol carrier binding protein (SCP-2)], FA transport protein (FATP), and glucose transporters 1 and 2 (GLUT1, GLUT2) insulin receptor. L-FABP gene ablation enhanced the concentration of SCP-2, SR-B1, FATP4, and GLUT1 in the cholesterol-poor microdomains, with functional implications in HDL-mediated uptake and efflux of cholesterol. Thus L-FABP gene ablation significantly impacted the proportion of cholesterol-rich versus -poor microdomains in the hepatocyte plasma membrane and altered the distribution of lipids and proteins involved in cholesterol uptake therein.
topic fatty acid
cholesterol
high density lipoprotein
lipids
liver
membranes
url http://www.sciencedirect.com/science/article/pii/S0022227520413628
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