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Publication : Sall1 is a transcriptional regulator defining microglia identity and function.

First Author  Buttgereit A Year  2016
Journal  Nat Immunol Volume  17
Issue  12 Pages  1397-1406
PubMed ID  27776109 Mgi Jnum  J:259946
Mgi Id  MGI:6141725 Doi  10.1038/ni.3585
Citation  Buttgereit A, et al. (2016) Sall1 is a transcriptional regulator defining microglia identity and function. Nat Immunol 17(12):1397-1406
abstractText  Microglia are the resident macrophages of the central nervous system (CNS). Gene expression profiling has identified Sall1, which encodes a transcriptional regulator, as a microglial signature gene. We found that Sall1 was expressed by microglia but not by other members of the mononuclear phagocyte system or by other CNS-resident cells. Using Sall1 for microglia-specific gene targeting, we found that the cytokine receptor CSF1R was involved in the maintenance of adult microglia and that the receptor for the cytokine TGF-beta suppressed activation of microglia. We then used the microglia-specific expression of Sall1 to inducibly inactivate the murine Sall1 locus in vivo, which resulted in the conversion of microglia from resting tissue macrophages into inflammatory phagocytes, leading to altered neurogenesis and disturbed tissue homeostasis. Collectively, our results show that transcriptional regulation by Sall1 maintains microglial identity and physiological properties in the CNS and allows microglia-specific manipulation in vivo.
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