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Daxx mediates activation‐induced cell death in microglia by triggering MST1 signalling
Author(s) -
Yun Hee Jae,
Yoon JeHyun,
Lee Jae Keun,
Noh KyungTae,
Yoon KyoungWan,
Oh Sang Phil,
Oh Hyun Jung,
Chae Ji Soo,
Hwang Sang Gil,
Kim Eun Hee,
Maul Gerd G,
Lim DaeSik,
Choi EuiJu
Publication year - 2011
Publication title -
the embo journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 7.484
H-Index - 392
eISSN - 1460-2075
pISSN - 0261-4189
DOI - 10.1038/emboj.2011.152
Subject(s) - biology , microglia , microbiology and biotechnology , programmed cell death , death associated protein 6 , signalling , apoptosis , immunology , nuclear protein , transcription factor , genetics , inflammation , gene
Microglia, the resident macrophages of the mammalian central nervous system, migrate to sites of tissue damage or infection and become activated. Although the persistent secretion of inflammatory mediators by the activated cells contributes to the pathogenesis of various neurological disorders, most activated microglia eventually undergo apoptosis through the process of activation‐induced cell death (AICD). The molecular mechanism of AICD, however, has remained unclear. Here, we show that Daxx and mammalian Ste20‐like kinase‐1 (MST1) mediate apoptosis elicited by interferon‐γ (IFN‐γ) in microglia. IFN‐γ upregulated the expression of Daxx, which in turn mediated the homodimerization, activation, and nuclear translocation of MST1 and apoptosis in microglial cells. Depletion of Daxx or MST1 by RNA interference also attenuated IFN‐γ‐induced cell death in primary rat microglia. Furthermore, the extent of IFN‐γ‐induced death of microglia in the brain of MST1‐null mice was significantly reduced compared with that apparent in wild‐type mice. Our results thus highlight new functions of Daxx and MST1 that they are the key mediators of microglial cell death initiated by the proinflammatory cytokine IFN‐γ.