Model-driven Multi-omic Data Analysis Elucidates Metabolic Immunomodulators of Macrophage Activation

Overview

Journal Mol Syst Biol

Specialty Molecular Biology

Date 2012 Jun 28

PMID 22735334

Citations 86

Authors

Aarash Bordbar

Monica L Mo

Ernesto S Nakayasu

Alexandra C Schrimpe-Rutledge

Young-Mo Kim

Thomas O Metz

Marcus B Jones

Bryan C Frank

Richard D Smith

Scott N Peterson

Daniel R Hyduke

Joshua N Adkins

Bernhard O Palsson

Affiliations

Soon will be listed here.

Abstract

Macrophages are central players in immune response, manifesting divergent phenotypes to control inflammation and innate immunity through release of cytokines and other signaling factors. Recently, the focus on metabolism has been reemphasized as critical signaling and regulatory pathways of human pathophysiology, ranging from cancer to aging, often converge on metabolic responses. Here, we used genome-scale modeling and multi-omics (transcriptomics, proteomics, and metabolomics) analysis to assess metabolic features that are critical for macrophage activation. We constructed a genome-scale metabolic network for the RAW 264.7 cell line to determine metabolic modulators of activation. Metabolites well-known to be associated with immunoactivation (glucose and arginine) and immunosuppression (tryptophan and vitamin D3) were among the most critical effectors. Intracellular metabolic mechanisms were assessed, identifying a suppressive role for de-novo nucleotide synthesis. Finally, underlying metabolic mechanisms of macrophage activation are identified by analyzing multi-omic data obtained from LPS-stimulated RAW cells in the context of our flux-based predictions. Our study demonstrates metabolism's role in regulating activation may be greater than previously anticipated and elucidates underlying connections between activation and metabolic effectors.

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