An environment-dependent transcriptional network specifies human microglia identity.
David GosselinDylan SkolaNicole G CoufalInge R HoltmanJohannes C M SchlachetzkiEniko SajtiBaptiste N JaegerCarolyn O'ConnorConor FitzpatrickMartina P PasillasMonique PenaAmy AdairDavid D GondaMichael L LevyRichard M RansohoffFred H GageChristopher K GlassPublished in: Science (New York, N.Y.) (2017)
Microglia play essential roles in central nervous system (CNS) homeostasis and influence diverse aspects of neuronal function. However, the transcriptional mechanisms that specify human microglia phenotypes are largely unknown. We examined the transcriptomes and epigenetic landscapes of human microglia isolated from surgically resected brain tissue ex vivo and after transition to an in vitro environment. Transfer to a tissue culture environment resulted in rapid and extensive down-regulation of microglia-specific genes that were induced in primitive mouse macrophages after migration into the fetal brain. Substantial subsets of these genes exhibited altered expression in neurodegenerative and behavioral diseases and were associated with noncoding risk variants. These findings reveal an environment-dependent transcriptional network specifying microglia-specific programs of gene expression and facilitate efforts to understand the roles of microglia in human brain diseases.
Keyphrases
- gene expression
- inflammatory response
- neuropathic pain
- endothelial cells
- genome wide
- dna methylation
- induced pluripotent stem cells
- transcription factor
- high glucose
- white matter
- resting state
- lymph node
- spinal cord
- multiple sclerosis
- single cell
- oxidative stress
- functional connectivity
- cerebral ischemia
- heat shock
- drug induced
- diabetic rats
- quality improvement