Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model

BACKGROUND: Activation of microglia, the resident immune cells of the central nervous system, is a prominent pathological hallmark of Alzheimer’s disease (AD). However, the gene expression changes underlying microglia activation in response to tau pathology remain elusive. Furthermore, it is not cle...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Hong, Li, Yupeng, Ryder, John W., Hole, Justin T., Ebert, Philip J., Airey, David C., Qian, Hui-Rong, Logsdon, Benjamin, Fisher, Alice, Ahmed, Zeshan, Murray, Tracey K., Cavallini, Annalisa, Bose, Suchira, Eastwood, Brian J., Collier, David A., Dage, Jeffrey L., Miller, Bradley B., Merchant, Kalpana M., O’Neill, Michael J., Demattos, Ronald B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6296031/
https://www.ncbi.nlm.nih.gov/pubmed/30558641
http://dx.doi.org/10.1186/s13024-018-0296-y
_version_ 1783380963768664064
author Wang, Hong
Li, Yupeng
Ryder, John W.
Hole, Justin T.
Ebert, Philip J.
Airey, David C.
Qian, Hui-Rong
Logsdon, Benjamin
Fisher, Alice
Ahmed, Zeshan
Murray, Tracey K.
Cavallini, Annalisa
Bose, Suchira
Eastwood, Brian J.
Collier, David A.
Dage, Jeffrey L.
Miller, Bradley B.
Merchant, Kalpana M.
O’Neill, Michael J.
Demattos, Ronald B.
author_facet Wang, Hong
Li, Yupeng
Ryder, John W.
Hole, Justin T.
Ebert, Philip J.
Airey, David C.
Qian, Hui-Rong
Logsdon, Benjamin
Fisher, Alice
Ahmed, Zeshan
Murray, Tracey K.
Cavallini, Annalisa
Bose, Suchira
Eastwood, Brian J.
Collier, David A.
Dage, Jeffrey L.
Miller, Bradley B.
Merchant, Kalpana M.
O’Neill, Michael J.
Demattos, Ronald B.
author_sort Wang, Hong
collection PubMed
description BACKGROUND: Activation of microglia, the resident immune cells of the central nervous system, is a prominent pathological hallmark of Alzheimer’s disease (AD). However, the gene expression changes underlying microglia activation in response to tau pathology remain elusive. Furthermore, it is not clear how murine gene expression changes relate to human gene expression networks. METHODS: Microglia cells were isolated from rTg4510 tau transgenic mice and gene expression was profiled using RNA sequencing. Four age groups of mice (2-, 4-, 6-, and 8-months) were analyzed to capture longitudinal gene expression changes that correspond to varying levels of pathology, from minimal tau accumulation to massive neuronal loss. Statistical and system biology approaches were used to analyze the genes and pathways that underlie microglia activation. Differentially expressed genes were compared to human brain co-expression networks. RESULTS: Statistical analysis of RNAseq data indicated that more than 4000 genes were differentially expressed in rTg4510 microglia compared to wild type microglia, with the majority of gene expression changes occurring between 2- and 4-months of age. These genes belong to four major clusters based on their temporal expression pattern. Genes involved in innate immunity were continuously up-regulated, whereas genes involved in the glutamatergic synapse were down-regulated. Up-regulated innate inflammatory pathways included NF-κB signaling, cytokine-cytokine receptor interaction, lysosome, oxidative phosphorylation, and phagosome. NF-κB and cytokine signaling were among the earliest pathways activated, likely driven by the RELA, STAT1 and STAT6 transcription factors. The expression of many AD associated genes such as APOE and TREM2 was also altered in rTg4510 microglia cells. Differentially expressed genes in rTg4510 microglia were enriched in human neurodegenerative disease associated pathways, including Alzheimer’s, Parkinson’s, and Huntington’s diseases, and highly overlapped with the microglia and endothelial modules of human brain transcriptional co-expression networks. CONCLUSION: This study revealed temporal transcriptome alterations in microglia cells in response to pathological tau perturbation and provides insight into the molecular changes underlying microglia activation during tau mediated neurodegeneration. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s13024-018-0296-y) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-6296031
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-62960312018-12-18 Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model Wang, Hong Li, Yupeng Ryder, John W. Hole, Justin T. Ebert, Philip J. Airey, David C. Qian, Hui-Rong Logsdon, Benjamin Fisher, Alice Ahmed, Zeshan Murray, Tracey K. Cavallini, Annalisa Bose, Suchira Eastwood, Brian J. Collier, David A. Dage, Jeffrey L. Miller, Bradley B. Merchant, Kalpana M. O’Neill, Michael J. Demattos, Ronald B. Mol Neurodegener Research Article BACKGROUND: Activation of microglia, the resident immune cells of the central nervous system, is a prominent pathological hallmark of Alzheimer’s disease (AD). However, the gene expression changes underlying microglia activation in response to tau pathology remain elusive. Furthermore, it is not clear how murine gene expression changes relate to human gene expression networks. METHODS: Microglia cells were isolated from rTg4510 tau transgenic mice and gene expression was profiled using RNA sequencing. Four age groups of mice (2-, 4-, 6-, and 8-months) were analyzed to capture longitudinal gene expression changes that correspond to varying levels of pathology, from minimal tau accumulation to massive neuronal loss. Statistical and system biology approaches were used to analyze the genes and pathways that underlie microglia activation. Differentially expressed genes were compared to human brain co-expression networks. RESULTS: Statistical analysis of RNAseq data indicated that more than 4000 genes were differentially expressed in rTg4510 microglia compared to wild type microglia, with the majority of gene expression changes occurring between 2- and 4-months of age. These genes belong to four major clusters based on their temporal expression pattern. Genes involved in innate immunity were continuously up-regulated, whereas genes involved in the glutamatergic synapse were down-regulated. Up-regulated innate inflammatory pathways included NF-κB signaling, cytokine-cytokine receptor interaction, lysosome, oxidative phosphorylation, and phagosome. NF-κB and cytokine signaling were among the earliest pathways activated, likely driven by the RELA, STAT1 and STAT6 transcription factors. The expression of many AD associated genes such as APOE and TREM2 was also altered in rTg4510 microglia cells. Differentially expressed genes in rTg4510 microglia were enriched in human neurodegenerative disease associated pathways, including Alzheimer’s, Parkinson’s, and Huntington’s diseases, and highly overlapped with the microglia and endothelial modules of human brain transcriptional co-expression networks. CONCLUSION: This study revealed temporal transcriptome alterations in microglia cells in response to pathological tau perturbation and provides insight into the molecular changes underlying microglia activation during tau mediated neurodegeneration. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s13024-018-0296-y) contains supplementary material, which is available to authorized users. BioMed Central 2018-12-17 /pmc/articles/PMC6296031/ /pubmed/30558641 http://dx.doi.org/10.1186/s13024-018-0296-y Text en © The Author(s). 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Wang, Hong
Li, Yupeng
Ryder, John W.
Hole, Justin T.
Ebert, Philip J.
Airey, David C.
Qian, Hui-Rong
Logsdon, Benjamin
Fisher, Alice
Ahmed, Zeshan
Murray, Tracey K.
Cavallini, Annalisa
Bose, Suchira
Eastwood, Brian J.
Collier, David A.
Dage, Jeffrey L.
Miller, Bradley B.
Merchant, Kalpana M.
O’Neill, Michael J.
Demattos, Ronald B.
Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title_full Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title_fullStr Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title_full_unstemmed Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title_short Genome-wide RNAseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rTg4510 tau transgenic animal model
title_sort genome-wide rnaseq study of the molecular mechanisms underlying microglia activation in response to pathological tau perturbation in the rtg4510 tau transgenic animal model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6296031/
https://www.ncbi.nlm.nih.gov/pubmed/30558641
http://dx.doi.org/10.1186/s13024-018-0296-y
work_keys_str_mv AT wanghong genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT liyupeng genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT ryderjohnw genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT holejustint genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT ebertphilipj genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT aireydavidc genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT qianhuirong genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT logsdonbenjamin genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT fisheralice genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT ahmedzeshan genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT murraytraceyk genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT cavalliniannalisa genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT bosesuchira genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT eastwoodbrianj genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT collierdavida genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT dagejeffreyl genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT millerbradleyb genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT merchantkalpanam genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT oneillmichaelj genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel
AT demattosronaldb genomewidernaseqstudyofthemolecularmechanismsunderlyingmicrogliaactivationinresponsetopathologicaltauperturbationinthertg4510tautransgenicanimalmodel

Ejemplares similares