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- The IKK-related kinase TBK1 activates mTORC1 directly in response to growth factors and innate immune agonists.
The IKK-related kinase TBK1 activates mTORC1 directly in response to growth factors and innate immune agonists.
Citation | “The Ikk-Related Kinase Tbk1 Activates Mtorc1 Directly In Response To Growth Factors And Innate Immune Agonists.”. The Embo Journal, pp. 19-38. . |
Center | University of Michigan |
Author | Cagri Bodur, Dubek Kazyken, Kezhen Huang, Bilgen Ekim Ustunel, Kate A Siroky, Aaron Seth Tooley, Ian E Gonzalez, Daniel H Foley, Hugo A Acosta-Jaquez, Tammy M Barnes, Gabrielle K Steinl, Kae-Won Cho, Carey N Lumeng, Steven M Riddle, Martin G Myers, Diane C Fingar |
Keywords | IFN‐β, TBK1, mTOR, mTORC1 |
Abstract |
The innate immune kinase TBK1 initiates inflammatory responses to combat infectious pathogens by driving production of type I interferons. TBK1 also controls metabolic processes and promotes oncogene-induced cell proliferation and survival. Here, we demonstrate that TBK1 activates mTOR complex 1 (mTORC1) directly. In cultured cells, TBK1 associates with and activates mTORC1 through site-specific mTOR phosphorylation (on S2159) in response to certain growth factor receptors (i.e., EGF-receptor but not insulin receptor) and pathogen recognition receptors (PRRs) (i.e., TLR3; TLR4), revealing a stimulus-selective role for TBK1 in mTORC1 regulation. By studying cultured macrophages and those isolated from genome edited mTOR S2159A knock-in mice, we show that mTOR S2159 phosphorylation promotes mTORC1 signaling, IRF3 nuclear translocation, and IFN-β production. These data demonstrate a direct mechanistic link between TBK1 and mTORC1 function as well as physiologic significance of the TBK1-mTORC1 axis in control of innate immune function. These data unveil TBK1 as a direct mTORC1 activator and suggest unanticipated roles for mTORC1 downstream of TBK1 in control of innate immunity, tumorigenesis, and disorders linked to chronic inflammation. |
Year of Publication |
2018
|
Journal |
The EMBO journal
|
Volume |
37
|
Issue |
1
|
Number of Pages |
19-38
|
Date Published |
12/2018
|
ISSN Number |
1460-2075
|
DOI |
10.15252/embj.201696164
|
Alternate Journal |
EMBO J.
|
PMID |
29150432
|
PMCID |
PMC5753041
|
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