Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance

BACKGROUND: The sequence of events leading to the development of insulin resistance (IR) as well as the underlying pathophysiological mechanisms are incompletely understood. As reductionist approaches have been largely unsuccessful in providing an understanding of the pathogenesis of IR, there is a...

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Autores principales: Kleemann, Robert, van Erk, Marjan, Verschuren, Lars, van den Hoek, Anita M., Koek, Maud, Wielinga, Peter Y., Jie, Annie, Pellis, Linette, Bobeldijk-Pastorova, Ivana, Kelder, Thomas, Toet, Karin, Wopereis, Suzan, Cnubben, Nicole, Evelo, Chris, van Ommen, Ben, Kooistra, Teake
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2809107/
https://www.ncbi.nlm.nih.gov/pubmed/20098690
http://dx.doi.org/10.1371/journal.pone.0008817
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author Kleemann, Robert
van Erk, Marjan
Verschuren, Lars
van den Hoek, Anita M.
Koek, Maud
Wielinga, Peter Y.
Jie, Annie
Pellis, Linette
Bobeldijk-Pastorova, Ivana
Kelder, Thomas
Toet, Karin
Wopereis, Suzan
Cnubben, Nicole
Evelo, Chris
van Ommen, Ben
Kooistra, Teake
author_facet Kleemann, Robert
van Erk, Marjan
Verschuren, Lars
van den Hoek, Anita M.
Koek, Maud
Wielinga, Peter Y.
Jie, Annie
Pellis, Linette
Bobeldijk-Pastorova, Ivana
Kelder, Thomas
Toet, Karin
Wopereis, Suzan
Cnubben, Nicole
Evelo, Chris
van Ommen, Ben
Kooistra, Teake
author_sort Kleemann, Robert
collection PubMed
description BACKGROUND: The sequence of events leading to the development of insulin resistance (IR) as well as the underlying pathophysiological mechanisms are incompletely understood. As reductionist approaches have been largely unsuccessful in providing an understanding of the pathogenesis of IR, there is a need for an integrative, time-resolved approach to elucidate the development of the disease. METHODOLOGY/PRINCIPAL FINDINGS: Male ApoE3Leiden transgenic mice exhibiting a humanized lipid metabolism were fed a high-fat diet (HFD) for 0, 1, 6, 9, or 12 weeks. Development of IR was monitored in individual mice over time by performing glucose tolerance tests and measuring specific biomarkers in plasma, and hyperinsulinemic-euglycemic clamp analysis to assess IR in a tissue-specific manner. To elucidate the dynamics and tissue-specificity of metabolic and inflammatory processes key to IR development, a time-resolved systems analysis of gene expression and metabolite levels in liver, white adipose tissue (WAT), and muscle was performed. During HFD feeding, the mice became increasingly obese and showed a gradual increase in glucose intolerance. IR became first manifest in liver (week 6) and then in WAT (week 12), while skeletal muscle remained insulin-sensitive. Microarray analysis showed rapid upregulation of carbohydrate (only liver) and lipid metabolism genes (liver, WAT). Metabolomics revealed significant changes in the ratio of saturated to polyunsaturated fatty acids (liver, WAT, plasma) and in the concentrations of glucose, gluconeogenesis and Krebs cycle metabolites, and branched amino acids (liver). HFD evoked an early hepatic inflammatory response which then gradually declined to near baseline. By contrast, inflammation in WAT increased over time, reaching highest values in week 12. In skeletal muscle, carbohydrate metabolism, lipid metabolism, and inflammation was gradually suppressed with HFD. CONCLUSIONS/SIGNIFICANCE: HFD-induced IR is a time- and tissue-dependent process that starts in liver and proceeds in WAT. IR development is paralleled by tissue-specific gene expression changes, metabolic adjustments, changes in lipid composition, and inflammatory responses in liver and WAT involving p65-NFkB and SOCS3. The alterations in skeletal muscle are largely opposite to those in liver and WAT.
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spelling pubmed-28091072010-01-23 Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance Kleemann, Robert van Erk, Marjan Verschuren, Lars van den Hoek, Anita M. Koek, Maud Wielinga, Peter Y. Jie, Annie Pellis, Linette Bobeldijk-Pastorova, Ivana Kelder, Thomas Toet, Karin Wopereis, Suzan Cnubben, Nicole Evelo, Chris van Ommen, Ben Kooistra, Teake PLoS One Research Article BACKGROUND: The sequence of events leading to the development of insulin resistance (IR) as well as the underlying pathophysiological mechanisms are incompletely understood. As reductionist approaches have been largely unsuccessful in providing an understanding of the pathogenesis of IR, there is a need for an integrative, time-resolved approach to elucidate the development of the disease. METHODOLOGY/PRINCIPAL FINDINGS: Male ApoE3Leiden transgenic mice exhibiting a humanized lipid metabolism were fed a high-fat diet (HFD) for 0, 1, 6, 9, or 12 weeks. Development of IR was monitored in individual mice over time by performing glucose tolerance tests and measuring specific biomarkers in plasma, and hyperinsulinemic-euglycemic clamp analysis to assess IR in a tissue-specific manner. To elucidate the dynamics and tissue-specificity of metabolic and inflammatory processes key to IR development, a time-resolved systems analysis of gene expression and metabolite levels in liver, white adipose tissue (WAT), and muscle was performed. During HFD feeding, the mice became increasingly obese and showed a gradual increase in glucose intolerance. IR became first manifest in liver (week 6) and then in WAT (week 12), while skeletal muscle remained insulin-sensitive. Microarray analysis showed rapid upregulation of carbohydrate (only liver) and lipid metabolism genes (liver, WAT). Metabolomics revealed significant changes in the ratio of saturated to polyunsaturated fatty acids (liver, WAT, plasma) and in the concentrations of glucose, gluconeogenesis and Krebs cycle metabolites, and branched amino acids (liver). HFD evoked an early hepatic inflammatory response which then gradually declined to near baseline. By contrast, inflammation in WAT increased over time, reaching highest values in week 12. In skeletal muscle, carbohydrate metabolism, lipid metabolism, and inflammation was gradually suppressed with HFD. CONCLUSIONS/SIGNIFICANCE: HFD-induced IR is a time- and tissue-dependent process that starts in liver and proceeds in WAT. IR development is paralleled by tissue-specific gene expression changes, metabolic adjustments, changes in lipid composition, and inflammatory responses in liver and WAT involving p65-NFkB and SOCS3. The alterations in skeletal muscle are largely opposite to those in liver and WAT. Public Library of Science 2010-01-21 /pmc/articles/PMC2809107/ /pubmed/20098690 http://dx.doi.org/10.1371/journal.pone.0008817 Text en Kleemann et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kleemann, Robert
van Erk, Marjan
Verschuren, Lars
van den Hoek, Anita M.
Koek, Maud
Wielinga, Peter Y.
Jie, Annie
Pellis, Linette
Bobeldijk-Pastorova, Ivana
Kelder, Thomas
Toet, Karin
Wopereis, Suzan
Cnubben, Nicole
Evelo, Chris
van Ommen, Ben
Kooistra, Teake
Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title_full Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title_fullStr Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title_full_unstemmed Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title_short Time-Resolved and Tissue-Specific Systems Analysis of the Pathogenesis of Insulin Resistance
title_sort time-resolved and tissue-specific systems analysis of the pathogenesis of insulin resistance
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2809107/
https://www.ncbi.nlm.nih.gov/pubmed/20098690
http://dx.doi.org/10.1371/journal.pone.0008817
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