Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes

Islet leukocytic infiltration (insulitis) is first obvious at around 4 weeks of age in the NOD mouse – a model for human type 1 diabetes (T1D). The molecular events that lead to insulitis and initiate autoimmune diabetes are poorly understood. Since TID is caused by numerous genes, we hypothesized t...

Descripción completa

Detalles Bibliográficos
Autores principales: Wu, Jian, Kakoola, Dorothy N., Lenchik, Nataliya I., Desiderio, Dominic M., Marshall, Dana R., Gerling, Ivan C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3469658/
https://www.ncbi.nlm.nih.gov/pubmed/23071669
http://dx.doi.org/10.1371/journal.pone.0046941
_version_ 1782246121920266240
author Wu, Jian
Kakoola, Dorothy N.
Lenchik, Nataliya I.
Desiderio, Dominic M.
Marshall, Dana R.
Gerling, Ivan C.
author_facet Wu, Jian
Kakoola, Dorothy N.
Lenchik, Nataliya I.
Desiderio, Dominic M.
Marshall, Dana R.
Gerling, Ivan C.
author_sort Wu, Jian
collection PubMed
description Islet leukocytic infiltration (insulitis) is first obvious at around 4 weeks of age in the NOD mouse – a model for human type 1 diabetes (T1D). The molecular events that lead to insulitis and initiate autoimmune diabetes are poorly understood. Since TID is caused by numerous genes, we hypothesized that multiple molecular pathways are altered and interact to initiate this disease. We evaluated the molecular phenotype (mRNA and protein expression) and molecular networks of ex vivo unfractionated spleen leukocytes from 2 and 4 week-old NOD mice in comparison to two control strains. Analysis of the global gene expression profiles and hierarchical clustering revealed that the majority (∼90%) of the differentially expressed genes in NOD mice were repressed. Furthermore, analysis using a modern suite of multiple bioinformatics approaches identified abnormal molecular pathways that can be divided broadly into 2 categories: metabolic pathways, which were predominant at 2 weeks, and immune response pathways, which were predominant at 4 weeks. Network analysis by Ingenuity pathway analysis identified key genes/molecules that may play a role in regulating these pathways. These included five that were common to both ages (TNF, HNF4A, IL15, Progesterone, and YWHAZ), and others that were unique to 2 weeks (e.g. MYC/MYCN, TGFB1, and IL2) and to 4 weeks (e.g. IFNG, beta-estradiol, p53, NFKB, AKT, PRKCA, IL12, and HLA-C). Based on the literature, genes that may play a role in regulating metabolic pathways at 2 weeks include Myc and HNF4A, and at 4 weeks, beta-estradiol, p53, Akt, HNF4A and AR. Our data suggest that abnormalities in regulation of metabolic pathways in the immune cells of young NOD mice lead to abnormalities in the immune response pathways and as such may play a role in the initiation of autoimmune diabetes. Thus, targeting metabolism may provide novel approaches to preventing and/or treating autoimmune diabetes.
format Online
Article
Text
id pubmed-3469658
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-34696582012-10-15 Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes Wu, Jian Kakoola, Dorothy N. Lenchik, Nataliya I. Desiderio, Dominic M. Marshall, Dana R. Gerling, Ivan C. PLoS One Research Article Islet leukocytic infiltration (insulitis) is first obvious at around 4 weeks of age in the NOD mouse – a model for human type 1 diabetes (T1D). The molecular events that lead to insulitis and initiate autoimmune diabetes are poorly understood. Since TID is caused by numerous genes, we hypothesized that multiple molecular pathways are altered and interact to initiate this disease. We evaluated the molecular phenotype (mRNA and protein expression) and molecular networks of ex vivo unfractionated spleen leukocytes from 2 and 4 week-old NOD mice in comparison to two control strains. Analysis of the global gene expression profiles and hierarchical clustering revealed that the majority (∼90%) of the differentially expressed genes in NOD mice were repressed. Furthermore, analysis using a modern suite of multiple bioinformatics approaches identified abnormal molecular pathways that can be divided broadly into 2 categories: metabolic pathways, which were predominant at 2 weeks, and immune response pathways, which were predominant at 4 weeks. Network analysis by Ingenuity pathway analysis identified key genes/molecules that may play a role in regulating these pathways. These included five that were common to both ages (TNF, HNF4A, IL15, Progesterone, and YWHAZ), and others that were unique to 2 weeks (e.g. MYC/MYCN, TGFB1, and IL2) and to 4 weeks (e.g. IFNG, beta-estradiol, p53, NFKB, AKT, PRKCA, IL12, and HLA-C). Based on the literature, genes that may play a role in regulating metabolic pathways at 2 weeks include Myc and HNF4A, and at 4 weeks, beta-estradiol, p53, Akt, HNF4A and AR. Our data suggest that abnormalities in regulation of metabolic pathways in the immune cells of young NOD mice lead to abnormalities in the immune response pathways and as such may play a role in the initiation of autoimmune diabetes. Thus, targeting metabolism may provide novel approaches to preventing and/or treating autoimmune diabetes. Public Library of Science 2012-10-11 /pmc/articles/PMC3469658/ /pubmed/23071669 http://dx.doi.org/10.1371/journal.pone.0046941 Text en © 2012 Wu 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
Wu, Jian
Kakoola, Dorothy N.
Lenchik, Nataliya I.
Desiderio, Dominic M.
Marshall, Dana R.
Gerling, Ivan C.
Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title_full Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title_fullStr Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title_full_unstemmed Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title_short Molecular Phenotyping of Immune Cells from Young NOD Mice Reveals Abnormal Metabolic Pathways in the Early Induction Phase of Autoimmune Diabetes
title_sort molecular phenotyping of immune cells from young nod mice reveals abnormal metabolic pathways in the early induction phase of autoimmune diabetes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3469658/
https://www.ncbi.nlm.nih.gov/pubmed/23071669
http://dx.doi.org/10.1371/journal.pone.0046941
work_keys_str_mv AT wujian molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes
AT kakooladorothyn molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes
AT lenchiknataliyai molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes
AT desideriodominicm molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes
AT marshalldanar molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes
AT gerlingivanc molecularphenotypingofimmunecellsfromyoungnodmicerevealsabnormalmetabolicpathwaysintheearlyinductionphaseofautoimmunediabetes

Ejemplares similares