Literature DB >> 21762917

Genetical genomics of Th1 and Th2 immune response in a baboon model of atherosclerosis risk factors.

A Vinson1, J E Curran, M P Johnson, T D Dyer, E K Moses, J Blangero, L A Cox, J Rogers, L M Havill, J L Vandeberg, M C Mahaney.   

Abstract

OBJECTIVE: CD4(+) T-cells mediate inflammation in atherosclerosis, but additive genetic effects on associated pathways of Th1 and Th2 immune response have not been described. We sought to characterize heritability, pleiotropy, and QTL effects on the expression of genes implicated in Th1 and Th2 immune response in a baboon model of risk factors for atherosclerosis.
METHODS: We employed a maximum likelihood-based variance decomposition approach to estimate additive genetic effects on transcript levels generated from a gene expression profile of lymphocytes in 499 pedigreed baboons maintained on a basal diet. Transcript levels for 57 genes implicated in Th1 and Th2 immune response were selected for analysis based on significant heritability in this profile. Multipoint whole genome scans were conducted on heritable transcript levels to localize QTLs influencing these measures. To evaluate pleiotropic effects on transcript levels, we estimated genetic and phenotypic correlations among transcript measures, and assessed their correspondence using a Mantel test. Network analysis using GeneGo's MetaCore™ software was conducted to characterize known interaction among coded proteins.
RESULTS: Heritabilities for candidate gene transcript levels ranged from 0.092-0.786 (median h(2)=0.278, P=4.72×10(-4)). Linkage analyses yielded significant evidence (LOD≥2.73) for 14 eQTLs (LOD score range 2.76-14.87, genome-wide P=4.9×10(-2)-1.03×10(-14)). Estimates of genetic correlation supported shared additive genetic effects incorporating all 57 transcripts (null hypothesis of ρ(G)=0 rejected at FDR≤0.05 for 522 of 1596 estimates), and accounted for most of the observed phenotypic correlation among transcripts (Mantel test, r([ρP],)([ρG])=0.781, P<0.0001). Network analysis revealed direct interactions among 54 of the 57 coded proteins.
CONCLUSIONS: We conclude that major genetic effects influence expression levels of multiple genes implicated in Th1 and Th2 immune response. Additionally, we find that expression levels of these candidate genes are characterized by extensive pleiotropy, consistent with known interaction among their coded proteins, many of which are independently associated with atherosclerosis.
Copyright © 2011 Elsevier Ireland Ltd. All rights reserved.

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Year:  2011        PMID: 21762917      PMCID: PMC3176804          DOI: 10.1016/j.atherosclerosis.2011.06.015

Source DB:  PubMed          Journal:  Atherosclerosis        ISSN: 0021-9150            Impact factor:   5.162


  35 in total

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Review 1.  Improving genome assemblies and annotations for nonhuman primates.

Authors:  Robert B Norgren
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Review 2.  Baboons as a model to study genetics and epigenetics of human disease.

Authors:  Laura A Cox; Anthony G Comuzzie; Lorena M Havill; Genesio M Karere; Kimberly D Spradling; Michael C Mahaney; Peter W Nathanielsz; Daniel P Nicolella; Robert E Shade; Saroja Voruganti; John L VandeBerg
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Review 3.  The value of extended pedigrees for next-generation analysis of complex disease in the rhesus macaque.

Authors:  Amanda Vinson; Kamm Prongay; Betsy Ferguson
Journal:  ILAR J       Date:  2013

4.  Th17 cells and IL-17 are involved in the disruption of vulnerable plaques triggered by short-term combination stimulation in apolipoprotein E-knockout mice.

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Journal:  Cell Mol Immunol       Date:  2013-04-01       Impact factor: 11.530

5.  The baboon kidney transcriptome: analysis of transcript sequence, splice variants, and abundance.

Authors:  Kimberly D Spradling; Jeremy P Glenn; Roy Garcia; Robert E Shade; Laura A Cox
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  5 in total

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