Systems Analysis of Eleven Rodent Disease Models Reveals an Inflammatome Signature and Key Drivers

Overview

Journal Mol Syst Biol

Specialty Molecular Biology

Date 2012 Jul 19

PMID 22806142

Citations 95

Authors

I-Ming Wang

Bin Zhang

Xia Yang

Jun Zhu

Serguei Stepaniants

Chunsheng Zhang

Qingying Meng

Mette Peters

Yudong He

Chester Ni

Deborah Slipetz

Michael A Crackower

Hani Houshyar

Christopher M Tan

Ernest Asante-Appiah

Gary ONeill

Mingjuan Jane Luo

Rolf Thieringer

Jeffrey Yuan

Chi-Sung Chiu

Pek Yee Lum

John Lamb

Yves Boie

Hilary A Wilkinson

Eric E Schadt

Hongyue Dai

Christopher Roberts

Affiliations

Soon will be listed here.

Abstract

Common inflammatome gene signatures as well as disease-specific signatures were identified by analyzing 12 expression profiling data sets derived from 9 different tissues isolated from 11 rodent inflammatory disease models. The inflammatome signature significantly overlaps with known drug targets and co-expressed gene modules linked to metabolic disorders and cancer. A large proportion of genes in this signature are tightly connected in tissue-specific Bayesian networks (BNs) built from multiple independent mouse and human cohorts. Both the inflammatome signature and the corresponding consensus BNs are highly enriched for immune response-related genes supported as causal for adiposity, adipokine, diabetes, aortic lesion, bone, muscle, and cholesterol traits, suggesting the causal nature of the inflammatome for a variety of diseases. Integration of this inflammatome signature with the BNs uncovered 151 key drivers that appeared to be more biologically important than the non-drivers in terms of their impact on disease phenotypes. The identification of this inflammatome signature, its network architecture, and key drivers not only highlights the shared etiology but also pinpoints potential targets for intervention of various common diseases.

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