Liver gene expression associated with diet and lesion development in atherosclerosis-prone mice: induction of components of alternative complement pathway

doi:10.1152/physiolgenomics.00146.2003

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Physiol. Genomics 19: 131-142, 2004. First published July 6, 2004; doi:10.1152/physiolgenomics.00146.2003
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Received 3 September 2003; accepted in final form 1 July 2004.
Physiological Genomics 19:131-142 (2004)
1094-8341/04 $5.00 © 2004 American Physiological Society

Liver gene expression associated with diet and lesion development in atherosclerosis-prone mice: induction of components of alternative complement pathway

Adrian Recinos, III ¹, Boyd K. Carr ¹, David B. Bartos ¹, Istvan Boldogh ², J. Russ Carmical ³, L. Maria Belalcazar ¹ and Allan R. Brasier ¹

¹ Department of Internal Medicine, University of Texas Medical Branch, Galveston, Texas 77555-1060
² Department of Microbiology and Immunology, University of Texas Medical Branch, Galveston, Texas 77555-1060
³ Sealy Center for Molecular Science, University of Texas Medical Branch, Galveston, Texas 77555-1060

Diet-induced changes in serum lipoproteins are a major riskfactor for the development of atherosclerosis, the leading causeof mortality in Westernized countries. Atherosclerosis is nowappreciated to be a systemic inflammatory disease where increasedsynthesis of inducible proteins by the liver, such as C-reactiveprotein (CRP) and others, may play roles in accelerating thedisease process. To systematically investigate the genetic responseof the liver to diet-induced atherosclerosis, we applied high-densitymicroarray technology in a mouse model of atherosclerosis (LDLR^–/–mouse). LDLR^–/– mice and congenic (LDLR^+/+) controlswere placed on low-fat (LF) or high-fat (HF) Western-style diets.The Western diet produced sustained elevations in total cholesterol(2.5-fold for LDLR^+/+, 5.0-fold LDLR^–/–) relativeto the respective LF groups. Tissues were harvested after 12wk when significant atherosclerotic lesion development was firstdetectable by en face histomorphometry of oil red O-stainedaortas. Diet, rather than genotype, was most highly associatedwith development of atherosclerotic lesions. Liver mRNA expressionprofiles of triplicate animals from each group were determinedby high-density oligonucleotide microarrays; and genes withtranscript levels influenced by genotype and diet were identifiedby two-way ANOVA. Approximately one-third of the 102 genes identifiedto be altered by diet [Pr(F) < 0.0005] were involved in lipidmetabolism. In addition, we identified components of the alternativecomplement pathway, including C3, properdin, and factor D, forwhich mRNA levels were independently confirmed by quantitativereal-time RT-PCR analysis, and C3 protein was demonstrated inaortic lesions by immunostaining. These findings suggest thatinduction of the alternative complement pathway may be an additionalmechanism by which a high-fat/Western diet accelerates atherosclerosis.

LDL receptor knockout mouse; microarray; factor D; adipsin; properdin; C3

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