Tank binding kinase 1 is a centrosome-associated kinase necessary for microtubule dynamics and mitosis

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作者
Smitha Pillai
Jonathan Nguyen
Joseph Johnson
Eric Haura
Domenico Coppola
Srikumar Chellappan
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[1] H. Lee Moffitt Cancer Center and Research Institute,Department of Tumor Biology
[2] H. Lee Moffitt Cancer Center and Research Institute,Department of Thoracic Oncology
[3] H. Lee Moffitt Cancer Center and Research Institute,Department of Anatomic Pathology
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TANK Binding Kinase 1 (TBK1) is a non-canonical IκB kinase that contributes to KRAS-driven lung cancer. Here we report that TBK1 plays essential roles in mammalian cell division. Specifically, levels of active phospho-TBK1 increase during mitosis and localize to centrosomes, mitotic spindles and midbody, and selective inhibition or silencing of TBK1 triggers defects in spindle assembly and prevents mitotic progression. TBK1 binds to the centrosomal protein CEP170 and to the mitotic apparatus protein NuMA, and both CEP170 and NuMA are TBK1 substrates. Further, TBK1 is necessary for CEP170 centrosomal localization and binding to the microtubule depolymerase Kif2b, and for NuMA binding to dynein. Finally, selective disruption of the TBK1–CEP170 complex augments microtubule stability and triggers defects in mitosis, suggesting that TBK1 functions as a mitotic kinase necessary for microtubule dynamics and mitosis.
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