1. Distinct functions of the dual leucine zipper kinase depending on its subcellular localization.
- Author
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Wallbach, Manuel, Duque Escobar, Jorge, Babaeikelishomi, Rohollah, Stahnke, Marie-Jeannette, Blume, Roland, Schröder, Sabine, Kruegel, Jenny, Maedler, Kathrin, Kluth, Oliver, Kehlenbach, Ralph H., Miosge, Nicolai, and Oetjen, Elke
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LEUCINE zippers , *APOPTOSIS , *TRANSCRIPTION factors , *TUMOR necrosis factors , *C-Jun N-terminal kinases , *CARRIER proteins , *CELLULAR signal transduction - Abstract
The dual leucine zipper kinase DLK induces β-cell apoptosis by inhibiting the transcriptional activity conferred by the β-cell protective transcription factor cAMP response element binding protein CREB. This action might contribute to β-cell loss and ultimately diabetes. Within its kinase domain DLK shares high homology with the mixed lineage kinase (MLK) 3, which is activated by tumor necrosis factor (TNF) α and interleukin (IL)-1β, known prediabetic signals. In the present study, the regulation of DLK in β-cells by these cytokines was investigated. Both, TNFα and IL-1β induced the nuclear translocation of DLK. Mutations within a putative nuclear localization signal (NLS) prevented basal and cytokine-induced nuclear localization of DLK and binding to the importin receptor importin α, thereby demonstrating a functional NLS within DLK. DLK NLS mutants were catalytically active as they phosphorylated their down-stream kinase c-Jun N-terminal kinase to the same extent as DLK wild-type but did neither inhibit CREB-dependent gene transcription nor transcription conferred by the promoter of the anti-apoptotic protein BCL-xL. In addition, the β-cell apoptosis-inducing effect of DLK was severely diminished by mutation of its NLS. In a murine model of prediabetes, enhanced nuclear DLK was found. These data demonstrate that DLK exerts distinct functions, depending on its subcellular localization and thus provide a novel level of regulating DLK action. Furthermore, the prevention of the nuclear localization of DLK as induced by prediabetic signals with consecutive suppression of β-cell apoptosis might constitute a novel target in the therapy of diabetes mellitus. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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