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Literature DB >> 9077551

Complex genetic control of HDL levels in mice in response to an atherogenic diet. Coordinate regulation of HDL levels and bile acid metabolism.

D Machleder¹, B Ivandic, C Welch, L Castellani, K Reue, A J Lusis.

Abstract

Inbred strains of mice differ in susceptibility to atherogenesis when challenged with a high fat, high cholesterol diet containing 0.5% cholic acid. Studies of recombinant inbred (RI) strains derived from the susceptible strain C57BL/6J (B6) and the resistant strains C3H/HeJ (C3H) and BALB/cJ have revealed an association between fatty streak lesion size and a decrease in high density lipoprotein (HDL) levels on the diet. To better understand the genetic factors contributing to HDL metabolism and atherogenesis in response to the diet, we studied mice derived from an intercross between B6 and C3H using a complete linkage map approach. A total of 185 female progeny were typed for 134 genetic markers spanning the mouse genome, resulting in an average interval of about 10 cM between markers. A locus on distal chromosome 1 containing the apolipoprotein AII gene was linked to HDL-cholesterol levels on both the chow and the atherogenic diets, but this locus did not contribute to the decrease in HDL-cholesterol in response to the diet. At least three distinct genetic loci, on chromosomes 3, 5, and 11, exhibited evidence of linkage to a decrease in HDL-cholesterol after a dietary challenge. Since a bile acid (cholic acid) is required for the diet induced changes in HDL levels and for atherogenesis in these strains, we examined cholesterol-7-alpha hydroxylase (C7AH) expression. Whereas B6 mice exhibited a large decrease in C7AH mRNA levels in response to the diet, C3H showed an increase. Among the intercross mice, multiple loci contributed to the regulation of C7AH mRNA levels in response to the diet, the most notable of which coincided with the loci on chromosomes 3, 5, and 11 controlling HDL levels in response to the diet. None of these loci were linked to the C7AH structural gene which we mapped to proximal chromosome 4. These studies reveal coordinate regulation of C7AH expression and HDL levels, and they indicate that the genetic factors controlling HDL levels are more complex than previously suggested by studies of RI strains. Furthermore, we observed that two of the loci for C7AH expression contributed to differences in gallstone formation between these strains.

Entities: Chemical Disease Gene Species

Mesh：

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Year: 1997 PMID： 9077551 PMCID： PMC507957 DOI： 10.1172/JCI119300

Source DB: PubMed Journal: J Clin Invest ISSN： 0021-9738 Impact factor: 14.808

55 in total

1. A genetic map of the mouse suitable for typing intraspecific crosses.

Authors: W Dietrich; H Katz; S E Lincoln; H S Shin; J Friedman; N C Dracopoli; E S Lander
Journal: Genetics Date: 1992-06 Impact factor: 4.562

2. A polymorphism affecting apolipoprotein A-II translational efficiency determines high density lipoprotein size and composition.

Authors: M H Doolittle; R C LeBoeuf; C H Warden; L M Bee; A J Lusis
Journal: J Biol Chem Date: 1990-09-25 Impact factor: 5.157

3. Regulation of hepatic cholesterol metabolism in humans: stimulatory effects of cholestyramine on HMG-CoA reductase activity and low density lipoprotein receptor expression in gallstone patients.

Authors: E Reihnér; B Angelin; M Rudling; S Ewerth; I Björkhem; K Einarsson
Journal: J Lipid Res Date: 1990-12 Impact factor: 5.922

4. Dietary cholesterol absorption, and sterol and bile acid excretion in hypercholesterolemia-resistant white rabbits.

Authors: M L Overturf; S A Smith; A M Gotto; J D Morrisett; T Tewson; J Poorman; D S Loose-Mitchell
Journal: J Lipid Res Date: 1990-11 Impact factor: 5.922

5. Bile acid sequestrants: mechanisms of action on bile acid and cholesterol metabolism.

Authors: K Einarsson; S Ericsson; S Ewerth; E Reihnér; M Rudling; D Ståhlberg; B Angelin
Journal: Eur J Clin Pharmacol Date: 1991 Impact factor: 2.953

6. Cloning of the human cholesterol 7 alpha-hydroxylase gene (CYP7) and localization to chromosome 8q11-q12.

Authors: J C Cohen; J J Cali; D F Jelinek; M Mehrabian; R S Sparkes; A J Lusis; D W Russell; H H Hobbs
Journal: Genomics Date: 1992-09 Impact factor: 5.736

7. Genetic and dietary interactions in the regulation of HMG-CoA reductase gene expression.

Authors: J J Hwa; S Zollman; C H Warden; B A Taylor; P A Edwards; A M Fogelman; A J Lusis
Journal: J Lipid Res Date: 1992-05 Impact factor: 5.922

8. Genetic regulation of cholesterol homeostasis: chromosomal organization of candidate genes.

Authors: C L Welch; Y R Xia; I Shechter; R Farese; M Mehrabian; S Mehdizadeh; C H Warden; A J Lusis
Journal: J Lipid Res Date: 1996-07 Impact factor: 5.922

9. Cholesterol metabolism in hypercholesterolemia-resistant rabbits.

Authors: D S Loose-Mitchell; J A Poorman; S A Smith; M L Overturf; J D Morrisett; A M Gotto; M R Soma
Journal: Atherosclerosis Date: 1991-04 Impact factor: 5.162

10. Antagonism between apolipoprotein AI regulatory protein 1, Ear3/COUP-TF, and hepatocyte nuclear factor 4 modulates apolipoprotein CIII gene expression in liver and intestinal cells.

Authors: M Mietus-Snyder; F M Sladek; G S Ginsburg; C F Kuo; J A Ladias; J E Darnell; S K Karathanasis
Journal: Mol Cell Biol Date: 1992-04 Impact factor: 4.272

35 in total

1. The effect of CYP7A1 polymorphisms on lipid responses to fenofibrate.

Authors: Jian Shen; Donna K Arnett; Laurence D Parnell; Chao-Qiang Lai; Robert J Straka; Paul N Hopkins; Ping An; Mary F Feitosa; José M Ordovás
Journal: J Cardiovasc Pharmacol Date: 2012-03 Impact factor: 3.105

2. Localization of atherosclerosis susceptibility loci to chromosomes 4 and 6 using the Ldlr knockout mouse model.

Authors: C L Welch; S Bretschger; N Latib; M Bezouevski; Y Guo; N Pleskac; C P Liang; C Barlow; H Dansky; J L Breslow; A R Tall
Journal: Proc Natl Acad Sci U S A Date: 2001-07-03 Impact factor: 11.205

3. Using advanced intercross lines for high-resolution mapping of HDL cholesterol quantitative trait loci.

Authors: Xiaosong Wang; Isabelle Le Roy; Edwige Nicodeme; Renhua Li; Richard Wagner; Christina Petros; Gary A Churchill; Stephen Harris; Ariel Darvasi; Jorge Kirilovsky; Pierre L Roubertoux; Beverly Paigen
Journal: Genome Res Date: 2003-06-12 Impact factor: 9.043

Complex genetic control of HDL levels in mice in response to an atherogenic diet. Coordinate regulation of HDL levels and bile acid metabolism.

1. A genetic map of the mouse suitable for typing intraspecific crosses.

2. A polymorphism affecting apolipoprotein A-II translational efficiency determines high density lipoprotein size and composition.

3. Regulation of hepatic cholesterol metabolism in humans: stimulatory effects of cholestyramine on HMG-CoA reductase activity and low density lipoprotein receptor expression in gallstone patients.

4. Dietary cholesterol absorption, and sterol and bile acid excretion in hypercholesterolemia-resistant white rabbits.

5. Bile acid sequestrants: mechanisms of action on bile acid and cholesterol metabolism.

6. Cloning of the human cholesterol 7 alpha-hydroxylase gene (CYP7) and localization to chromosome 8q11-q12.

7. Genetic and dietary interactions in the regulation of HMG-CoA reductase gene expression.

8. Genetic regulation of cholesterol homeostasis: chromosomal organization of candidate genes.

9. Cholesterol metabolism in hypercholesterolemia-resistant rabbits.

10. Antagonism between apolipoprotein AI regulatory protein 1, Ear3/COUP-TF, and hepatocyte nuclear factor 4 modulates apolipoprotein CIII gene expression in liver and intestinal cells.

1. The effect of CYP7A1 polymorphisms on lipid responses to fenofibrate.

2. Localization of atherosclerosis susceptibility loci to chromosomes 4 and 6 using the Ldlr knockout mouse model.

3. Using advanced intercross lines for high-resolution mapping of HDL cholesterol quantitative trait loci.

4. A large-sample QTL study in mice: II. Body composition.

5. High-resolution association mapping of atherosclerosis loci in mice.

6. Four additional mouse crosses improve the lipid QTL landscape and identify Lipg as a QTL gene.

7. Srb1 maps to mouse chromosome 5 in a region harboring putative QTLs for plasma lipoprotein levels.

Review 8. Integrating genetic and gene expression data: application to cardiovascular and metabolic traits in mice.

9. Haplotype analysis in multiple crosses to identify a QTL gene.

Review 10. Genetic analysis of cholesterol gallstone formation: searching for Lith (gallstone) genes.