Microglia emerge from erythromyeloid precursors via Pu.1- and Irf8-dependent pathways

Kierdorf, Katrin; Erny, Daniel; Goldmann, Tobias; Sander, Victor; Schulz, Christian; Perdiguero, Elisa Gomez; Wieghofer, Peter; Heinrich, Annette; Riemke, Pia; Hölscher, Christoph; Müller, Dominik; Luckow, Bruno; Brocker, Thomas; Debowski, Katharina; Fritz, Günter; Opdenakker, Ghislain; Diefenbach, Andreas; Biber, Knut; Heikenwälder, Mathias; Geissmann, Frédéric; Rosenbauer, Frank; Prinz, Marco

doi:10.1038/nn.3318

Cited by 1,139 publications

(1,135 citation statements)

References 35 publications

Supporting

Mentioning

1,085

Contrasting

Unclassified

Order By: Relevance

“…We have previously reported that IRF8 is expressed specifically in microglia in the CNS and plays a central role in regulating microglial gene expression [5]. Furthermore, recent studies have also shown that IRF8 is required for the full maturation of microglia [17] in addition to its physiological functions, including phagocytosis and cytokine production [18,19]. These observations led us to speculate that IRF8 may regulate microglial motility by controlling an expression pattern of microglial genes.…”

Section: Introductionmentioning

confidence: 92%

IRF8 is a transcriptional determinant for microglial motility

Masuda

Nishimoto

Tomiyama

et al. 2014

Purinergic Signalling

View full text Add to dashboard Cite

Microglia, the resident immune cells of the central nervous system, are constitutively mobile cells that undergo rapid directional movement toward sites of tissue disruption. However, transcriptional regulatory mechanisms of microglial motility remain unknown. In the present study, we show that interferon regulatory factor-8 (IRF8) regulates microglial motility. We found that ATP and complement component, C5a, induced chemotaxis of IRF8 wild-type microglia. However, these responses were markedly suppressed in microglia lacking IRF8 (Irf8 −/− ). In a consistent manner, phosphorylation of Akt (which plays a crucial role in ATP-induced chemotaxis) was abolished in Irf8 −/− microglia. Real-time polymerase chain reaction analysis revealed that motility-related microglial genes such as P2Y 12 receptor were significantly suppressed in Irf8 −/− microglia. Furthermore, Irf8 −/− microglia exhibited a differential expression pattern of nucleotidedegrading enzymes compared with their wild-type counterparts. Overall, our findings suggest that IRF8 may regulate microglial motility via the control of microglial gene expression.

show abstract

Section: Introductionmentioning

confidence: 92%

IRF8 is a transcriptional determinant for microglial motility

Masuda

Nishimoto

Tomiyama

et al. 2014

Purinergic Signalling

View full text Add to dashboard Cite

show abstract

“…They arise in the brain from early development and persist into adulthood. A long-standing controversy regarding the ontology of microglia led to a view that a subset of primitive myeloid precursors localized in the yolk sac give rise to early microglia [35][36][37]. Microglial precursors express CX3CR1 and CD45 and travel to the neuroectoderm in a matrix metalloproteinase-8-and matrix metalloproteinase-9-dependent manner [36,38].…”

Section: Microgliamentioning

confidence: 99%

“…A long-standing controversy regarding the ontology of microglia led to a view that a subset of primitive myeloid precursors localized in the yolk sac give rise to early microglia [35][36][37]. Microglial precursors express CX3CR1 and CD45 and travel to the neuroectoderm in a matrix metalloproteinase-8-and matrix metalloproteinase-9-dependent manner [36,38]. Importantly, these are not exchanged with fetal liver or bone marrowderived hematopoietic stem cells and they possess selfrenewing capability under physiologic conditions [35,36,39,40].…”

Section: Microgliamentioning

confidence: 99%

“…Microglial precursors express CX3CR1 and CD45 and travel to the neuroectoderm in a matrix metalloproteinase-8-and matrix metalloproteinase-9-dependent manner [36,38]. Importantly, these are not exchanged with fetal liver or bone marrowderived hematopoietic stem cells and they possess selfrenewing capability under physiologic conditions [35,36,39,40]. The morphology and protein expression of microglia are not uniform, and this heterogeneity could explain differential microglial responses in different surroundings [41,42].…”

Section: Microgliamentioning

confidence: 99%

See 1 more Smart Citation

Microglia and Monocyte-Derived Macrophages in Stroke

2016

View full text Add to dashboard Cite

Historically, the brain has been considered an immune-privileged organ separated from the peripheral immune system by the blood-brain barrier. However, immune responses do occur in the brain in neurological conditions in which the integrity of the blood-brain barrier is compromised, exposing the brain to peripheral antigens and endogenous danger signals. While most of the associated pathological processes occur in the central nervous system, it is now clear that peripheral immune cells, especially mononuclear phagocytes, that infiltrate into the injury site play a key role in modulating the progression of primary brain injury development. As inflammation is a necessary and critical component for the subsequent injury resolution process, understanding the contribution of mononuclear phagocytes on the regulation of inflammatory responses may provide novel approaches for potential therapies. Furthermore, predisposed comorbid conditions at the time of stroke cause the alteration of stroke-induced immune and inflammatory responses and subsequently influence stroke outcome. In this review, we summarize a role for microglia and monocytes/macrophages in acute ischemic stroke in the context of normal and metabolically compromised conditions.

show abstract

“…Microglia, the resident macrophages of the brain, are derived from early yolk sac macrophage progenitors (Ginhoux et al ., 2010; Kierdorf et al ., 2013). Under physiological conditions, there is negligible infiltration of peripheral monocytes to the brain parenchyma and the microglia population is likely sustained by self‐renewal (Ajami et al ., 2007).…”

Section: Introductionmentioning

confidence: 99%

Enhanced microglial pro‐inflammatory response to lipopolysaccharide correlates with brain infiltration and blood–brain barrier dysregulation in a mouse model of telomere shortening

et al. 2015

View full text Add to dashboard Cite

SummaryMicroglia are a proliferative population of resident brain macrophages that under physiological conditions self‐renew independent of hematopoiesis. Microglia are innate immune cells actively surveying the brain and are the earliest responders to injury. During aging, microglia elicit an enhanced innate immune response also referred to as ‘priming’. To date, it remains unknown whether telomere shortening affects the proliferative capacity and induces priming of microglia. We addressed this issue using early (first‐generation G1 mTerc−/−)‐ and late‐generation (third‐generation G3 and G4 mTerc−/−) telomerase‐deficient mice, which carry a homozygous deletion for the telomerase RNA component gene (mTerc). Late‐generation mTerc−/− microglia show telomere shortening and decreased proliferation efficiency. Under physiological conditions, gene expression and functionality of G3 mTerc−/− microglia are comparable with microglia derived from G1 mTerc−/− mice despite changes in morphology. However, after intraperitoneal injection of bacterial lipopolysaccharide (LPS), G3 mTerc−/− microglia mice show an enhanced pro‐inflammatory response. Nevertheless, this enhanced inflammatory response was not accompanied by an increased expression of genes known to be associated with age‐associated microglia priming. The increased inflammatory response in microglia correlates closely with increased peripheral inflammation, a loss of blood–brain barrier integrity, and infiltration of immune cells in the brain parenchyma in this mouse model of telomere shortening.

show abstract

Microglia emerge from erythromyeloid precursors via Pu.1- and Irf8-dependent pathways

Cited by 1,139 publications

References 35 publications

IRF8 is a transcriptional determinant for microglial motility

IRF8 is a transcriptional determinant for microglial motility

Microglia and Monocyte-Derived Macrophages in Stroke

Enhanced microglial pro‐inflammatory response to lipopolysaccharide correlates with brain infiltration and blood–brain barrier dysregulation in a mouse model of telomere shortening

Contact Info

Product

Resources

About