TY - JOUR
T1 - Transcriptome analysis of microglia in a mouse model of Rett syndrome
T2 - differential expression of genes associated with microglia/macrophage activation and cellular stress
AU - Zhao, Dejian
AU - Mokhtari, Ryan
AU - Pedrosa, Erika
AU - Birnbaum, Rayna
AU - Zheng, Deyou
AU - Lachman, Herbert M.
N1 - Funding Information:
This work was supported by grants from the National Institute of Mental Health (NIMH); MH099452 to DZ (Zheng) and MH099427 and MH087840 to HML. We are grateful to the New York State Department of Health (NYSTEM Program) for shared facility grant support (C029154). This project was made possible by support from the Albert Einstein College of Medicine’s Rose F. Kennedy Intellectual and Developmental Disabilities Research Center and by the National Institutes of Health’s National Institute of Child Health and Human Development (NIH/NICHD) grant P30 HD071593.
Funding Information:
The authors would like to acknowledge the Flow Cytometry Core Facility at Einstein, which is supported by the Einstein National Cancer Institute’s cancer center grant P30CA013330.
Publisher Copyright:
© 2017 The Author(s).
PY - 2017/3/29
Y1 - 2017/3/29
N2 - Background: Rett syndrome (RTT) is a severe, neurodevelopmental disorder primarily affecting girls, characterized by progressive loss of cognitive, social, and motor skills after a relatively brief period of typical development. It is usually due to de novo loss of function mutations in the X-linked gene, MeCP2, which codes for the gene expression and chromatin regulator, methyl-CpG binding protein 2. Although the behavioral phenotype appears to be primarily due to neuronal Mecp2 deficiency in mice, other cell types, including astrocytes and oligodendrocytes, also appear to contribute to some aspects of the RTT phenotype. In addition, microglia may also play a role. However, the effect of Mecp2 deficiency in microglia on RTT pathogenesis is controversial. Methods: In the current study, we applied whole transcriptome analysis using RNA-seq to gain insight into molecular pathways in microglia that might be dysregulated during the transition, in female mice heterozygous for an Mecp2-null allele (Mecp2 +/−; Het), from the pre-phenotypic (5 weeks) to the phenotypic phases (24 weeks). Results: We found a significant overlap in differentially expressed genes (DEGs) with genes involved in regulating the extracellular matrix, and those that are activated or inhibited when macrophages and microglia are stimulated towards the M1 and M2 activation states. However, the M1- and M2-associated genes were different in the 5- and 24-week samples. In addition, a substantial decrease in the expression of nine members of the heat shock protein (HSP) family was found in the 5-week samples, but not at 24 weeks. Conclusions: These findings suggest that microglia from pre-phenotypic and phenotypic female mice are activated in a manner different from controls and that pre-phenotypic female mice may have alterations in their capacity to response to heat stress and other stressors that function through the HSP pathway.
AB - Background: Rett syndrome (RTT) is a severe, neurodevelopmental disorder primarily affecting girls, characterized by progressive loss of cognitive, social, and motor skills after a relatively brief period of typical development. It is usually due to de novo loss of function mutations in the X-linked gene, MeCP2, which codes for the gene expression and chromatin regulator, methyl-CpG binding protein 2. Although the behavioral phenotype appears to be primarily due to neuronal Mecp2 deficiency in mice, other cell types, including astrocytes and oligodendrocytes, also appear to contribute to some aspects of the RTT phenotype. In addition, microglia may also play a role. However, the effect of Mecp2 deficiency in microglia on RTT pathogenesis is controversial. Methods: In the current study, we applied whole transcriptome analysis using RNA-seq to gain insight into molecular pathways in microglia that might be dysregulated during the transition, in female mice heterozygous for an Mecp2-null allele (Mecp2 +/−; Het), from the pre-phenotypic (5 weeks) to the phenotypic phases (24 weeks). Results: We found a significant overlap in differentially expressed genes (DEGs) with genes involved in regulating the extracellular matrix, and those that are activated or inhibited when macrophages and microglia are stimulated towards the M1 and M2 activation states. However, the M1- and M2-associated genes were different in the 5- and 24-week samples. In addition, a substantial decrease in the expression of nine members of the heat shock protein (HSP) family was found in the 5-week samples, but not at 24 weeks. Conclusions: These findings suggest that microglia from pre-phenotypic and phenotypic female mice are activated in a manner different from controls and that pre-phenotypic female mice may have alterations in their capacity to response to heat stress and other stressors that function through the HSP pathway.
KW - Autism
KW - Heat shock
KW - Innate immune system
KW - M1 activation
KW - M2 activation
KW - Microglia
KW - Rett syndrome
KW - Schizophrenia
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UR - http://www.scopus.com/inward/citedby.url?scp=85016243355&partnerID=8YFLogxK
U2 - 10.1186/s13229-017-0134-z
DO - 10.1186/s13229-017-0134-z
M3 - Article
C2 - 28367307
AN - SCOPUS:85016243355
SN - 2040-2392
VL - 8
JO - Molecular Autism
JF - Molecular Autism
IS - 1
M1 - 17
ER -
