- Main
Human microglia maturation is underpinned by specific gene regulatory networks.
- Han, Claudia;
- Li, Rick;
- Hansen, Emily;
- Trescott, Samantha;
- Fixsen, Bethany;
- Nguyen, Celina;
- Mora, Cristina;
- Spann, Nathanael;
- Bennett, Hunter;
- Poirion, Olivier;
- Buchanan, Justin;
- Warden, Anna;
- Xia, Bing;
- Schlachetzki, Johannes;
- Pasillas, Martina;
- Preissl, Sebastian;
- Wang, Allen;
- OConnor, Carolyn;
- Shriram, Shreya;
- Kim, Roy;
- Schafer, Danielle;
- Ramirez, Gabriela;
- Challacombe, Jean;
- Anavim, Samuel;
- Johnson, Avalon;
- Gupta, Mihir;
- Glass, Ian;
- Levy, Michael;
- Haim, Sharona;
- Gonda, David;
- Laurent, Louise;
- Hughes, Jennifer;
- Page, David;
- Blurton-Jones, Mathew;
- Glass, Christopher;
- Coufal, Nicole
- et al.
Abstract
Microglia phenotypes are highly regulated by the brain environment, but the transcriptional networks that specify the maturation of human microglia are poorly understood. Here, we characterized stage-specific transcriptomes and epigenetic landscapes of fetal and postnatal human microglia and acquired corresponding data in induced pluripotent stem cell (iPSC)-derived microglia, in cerebral organoids, and following engraftment into humanized mice. Parallel development of computational approaches that considered transcription factor (TF) co-occurrence and enhancer activity allowed prediction of shared and state-specific gene regulatory networks associated with fetal and postnatal microglia. Additionally, many features of the human fetal-to-postnatal transition were recapitulated in a time-dependent manner following the engraftment of iPSC cells into humanized mice. These data and accompanying computational approaches will facilitate further efforts to elucidate mechanisms by which human microglia acquire stage- and disease-specific phenotypes.
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