Abstract

The major hypotheses of this competing continuation application are: Ethanol exposure down-regulates alpha-2,6-sialyltransferase (2,6-ST) at the molecular level leading to defective glycosylation of apolipoprotein E (ApoE) and its association with HDL. Ethanol also affects sphingomyelin (SPM) and other phospholipids (PL) of HDL. These defects lead to impaired reverse cholesterol transport (RCT) that are reversed by low dietary omega 3-faty acids (omega 3FA). This laboratory has the following published (10 publication & 1 review) and preliminary data in support of the above hypotheses: 1. Ethanol impaired sialylation of both transferring (Tf) and ApoE by down-regulating 2,6-ST and its mRNA. 2. Both 2,6-ST-mRNA and GAPDH mRNA levels seemed to be intact in two autopsy liver samples from non-alcoholic controls. 3. Ethanol at 50 and 100mM decreased ST mRNA in human HepG2 cells stably expressing Cyp2E (Cyp2E cells) and high alcohol dehydrogenase (ADH cells), but not in Wild type. 4. However, acetaldehyde (Ach) at 50muM concentration decreased 2,6-ST mRNA even in Wilde type. 5. Ethanol destabilized liver 2,6-STmRNA, presumably via cis and trans- acting factors. 6. Desialylated ApoE had low affinity for HDL resulting in its impaired RCT function in both human and rat. 7. HDLs from both chronic ethanol-fed rats and human alcoholics showed defective RCT. 8. Very low dietary omega 3FA restored ethanol-mediated inhibition of RCT capacity of HDL. 9. Both 20:5 and 22:6 omega 3FA contents of HDL increased 4-4.7-fold in omega 3FA-fed group compared to the control group. 10. Sphingomyelin (SPM) content of HDL was decreased in ethanol group with concomitant inhibition of RCT. 11. HDLs from chronic human alcoholics also had lower HDL SPM compared to non-drinkers. 12. HDL devoid of SPM showed impaired RCT function. Therefore, the following specific aims are proposed to test hypotheses to understand the mechanisms of actions of alcohol and omega 3FA: Glycosylation:
Specific Aim 1 : Are protein factors involved in the ethanol-mediated destabilization of liver 2,6-ST mRNA? How does ethanol affect the distribution of 2,6-ST protein & its mRNA? Do livers from human alcoholics also exhibit decreased 2,6-ST protein & its mRNA? Specific Aim 2: Can the effects of ethanol in vivo be mimicked in human liver cell systems? Is active metabolism of ethanol a prerequisite for its effects in these cell systems? What are the cis and trans factors responsible for destabilizing 2,6-ST mRNA? Is Ach responsible for these effects at clinically relevant levels? Functional Consequences:
Specific Aim 3 : How do omega 3 FA alter ethanol-mediated defects in the RCT function of HDL? Specific Aim 4: Does ethanol affect the HDL SPM and other PL? Do human alcoholics have altered SPM and other PL levels in their HDL? Does ethanol-induced loss of SPM and other PL? Do human alcoholics have altered SPM and other PL levels in their HDL? Does ethanol-induced loss of SPM and other PL from HDL affect its RCT function? The laboratory will accomplish these in human and animal systems using molecular biology, immunochemical and biochemical approaches.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA008149-12
Application #
6509176
Study Section
Alcohol and Toxicology Subcommittee 4 (ALTX)
Program Officer
Purohit, Vishnu
Project Start
1992-12-01
Project End
2005-03-31
Budget Start
2002-04-01
Budget End
2003-03-31
Support Year
12
Fiscal Year
2002
Total Cost
$311,472
Indirect Cost

  Institution

Name
George Washington University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Washington
State
DC
Country
United States
Zip Code
20052

  Publications

Gong, Maokai; Castillo, Leslie; Redman, Robert S et al. (2008) Down-regulation of liver Galbeta1, 4GlcNAc alpha2, 6-sialyltransferase gene by ethanol significantly correlates with alcoholic steatosis in humans. Metabolism 57:1663-8
Gong, Maokai; Garige, Mamatha; Hirsch, Kenneth et al. (2007) Liver Galbeta1,4GlcNAc alpha2,6-sialyltransferase is down-regulated in human alcoholics: possible cause for the appearance of asialoconjugates. Metabolism 56:1241-7
Marmillot, Philippe; Patel, Sanket; Lakshman, M Raj (2007) Reverse cholesterol transport is regulated by varying fatty acyl chain saturation and sphingomyelin content in reconstituted high-density lipoproteins. Metabolism 56:251-9
Marmillot, Philippe; Munoz, Jennifer; Patel, Sanket et al. (2007) Long-term ethanol consumption impairs reverse cholesterol transport function of high-density lipoproteins by depleting high-density lipoprotein sphingomyelin both in rats and in humans. Metabolism 56:947-53
Azuine, Magnus A; Patel, Sanket J; Lakshman, M Raj (2006) Effects of chronic ethanol administration on the activities and relative synthetic rates of myelin and synaptosomal plasma membrane-associated sialidase in the rat brain. Neurochem Int 48:67-74
Garige, Mamatha; Azuine, Magnus A; Lakshman, M Raj (2006) Chronic ethanol consumption down-regulates CMP-NeuAc:GM3 alpha 2,8-sialyltransferase (ST8Sia-1) gene in the rat brain. Neurochem Int 49:312-8
Garige, Mamatha; Gong, Maokai; Lakshman, M Raj (2006) Ethanol destabilizes liver Gal beta l, 4GlcNAc alpha2,6-sialyltransferase, mRNA by depleting a 3'-untranslated region-specific binding protein. J Pharmacol Exp Ther 318:1076-82
Garige, Mamatha; Azuine, Magnus A; Lakshman, M Raj (2006) Chronic ethanol consumption upregulates the cytosolic and plasma membrane sialidase genes, but down regulates lysosomal membrane sialidase gene in rat liver. Metabolism 55:803-10
Azuine, Magnus A; Patel, Sanket J; Lakshman, M Raj (2005) Chronic ethanol feeding controls the activities of various sialidases by regulating their relative synthetic rates in the rat liver. Metabolism 54:1056-64
Garige, Mamatha; Gong, Maokai; Rao, Manjunath N et al. (2005) Mechanism of action of ethanol in the down-regulation of Gal(beta)1, 4GlcNAc alpha2,6-sialyltransferase messenger RNA in human liver cell lines. Metabolism 54:729-34

Showing the most recent 10 out of 18 publications