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  4. Broad-Ranging Natural Metabotype Variation Drives Physiological Plasticity in Healthy Control Inbred Rat Strains
 
research article

Broad-Ranging Natural Metabotype Variation Drives Physiological Plasticity in Healthy Control Inbred Rat Strains

Pontoizeau, Clement
•
Fearnside, Jane F.
•
Nayratil, Vincent
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2011
JOURNAL OF PROTEOME RESEARCH

Maintaining homeostasis in higher organisms involves a complex interplay of multiple ubiquitous and organ-specific molecular mechanisms that can be characterized using functional genomics technologies such as transcriptomics, proteomics, and metabonomics and dissected out through genetic investigations in healthy and diseased individuals. We characterized the genomic, metabolic, and physiological divergence of several inbred rat strains-Brown Norway, Lewis, Wistar Kyoto, Fisher (F344)-frequently used as healthy controls in genetic studies of the cardiometabolic syndrome. Hierarchical clustering of H-1 NMR-based metabolic profiles (n = 20 for urine, n = 16 for plasma) identified metabolic phenotype (metabotype) divergence patterns similar to the phylogenetic variability based on single nucleotide polymorphisms. However, the observed urinary metabotype variation exceeded that explainable by genetic polymorphisms. To understand further this natural variation, we used an integrative, knowledge-based network biology metabolic pathway analysis approach, coined Metabolite-Set Enrichment Analysis (MSEA). MSEA reveals that homeostasis and physiological plasticity can be achieved despite widespread divergences in glucose, lipid, amino acid, and energy metabolism in the host, together with different gut microbiota contributions suggestive of strain-specific transgenomic interactions. This work illustrates the concept of natural metabolomic variation, leading to physiologically stable albeit diverse strategies within the range of normality, all of which are highly relevant to animal model physiology, genetical genomics, and patient stratification in personalized healthcare.

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Type
research article
DOI
10.1021/pr101000z
Web of Science ID

WOS:000288924000022

Author(s)
Pontoizeau, Clement
Fearnside, Jane F.
Nayratil, Vincent
Domange, Celine
Cazier, Jean-Baptiste
Fernandez-Santamaria, Cristina
Kaisaki, Pamela J.
Emsley, Lyndon  
Toulhoat, Pierre
Bihoreau, Marie-Therese
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Date Issued

2011

Publisher

AMER CHEMICAL SOC

Published in
JOURNAL OF PROTEOME RESEARCH
Volume

10

Issue

4

Start page

1675

End page

1689

Subjects

metabonomics/metabolomics

•

natural variation

•

NMR spectroscopy

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metabolite-set enrichment analysis

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pathway analysis

•

cardiometabolic syndrome

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single nucleotide polymorphism

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
LRM  
Available on Infoscience
January 8, 2015
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/110005
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