IRF8 and MAFB drive distinct transcriptional machineries in different resident macrophages of the central nervous system.
Ayato YamasakiIroha ImanishiKaori TanakaYasuyuki OhkawaMakoto TsudaTakahiro MasudaPublished in: Communications biology (2024)
The central nervous system (CNS) includes anatomically distinct macrophage populations including parenchyma microglia and CNS-associated macrophages (CAMs) localized at the interfaces like meninges and perivascular space, which play specialized roles for the maintenance of the CNS homeostasis with the help of precisely controlled gene expressions. However, the transcriptional machinery that determines their cell-type specific states of microglia and CAMs remains poorly understood. Here we show, by myeloid cell-specific deletion of transcription factors, IRF8 and MAFB, that both adult microglia and CAMs utilize IRF8 to maintain their core gene signatures, although the genes altered by IRF8 deletion are different in the two macrophage populations. By contrast, MAFB deficiency robustly affected the gene expression profile of adult microglia, whereas CAMs are almost independent of MAFB. Our data suggest that distinct transcriptional machineries regulate different macrophages in the CNS.
Keyphrases
- genome wide identification
- transcription factor
- genome wide
- dendritic cells
- inflammatory response
- blood brain barrier
- neuropathic pain
- copy number
- gene expression
- dna methylation
- adipose tissue
- magnetic resonance
- dna binding
- bone marrow
- cerebrospinal fluid
- single cell
- spinal cord injury
- spinal cord
- immune response
- cell therapy
- palliative care
- replacement therapy
- stem cells
- big data
- contrast enhanced
- deep learning
- genetic diversity
- quality improvement
- artificial intelligence
- heat shock protein