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KMID : 0613820220320030241
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Journal of Life Science
2022 Volume.32 No. 3 p.241 ~ p.248
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IKK¥ã Facilitates the Activation of NF-¥êB by Hsp90
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Lee Jeong-Ah
Kim Dong-Wan
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Abstract
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NF-¥êB acts as a critical transcription factor in inflammation and innate immunity, and it is also closely involved in cell survival and tumorigenesis via induction of anti-apoptotic genes. In these processes, NF-¥êB cooperates with multiple other signaling molecules and pathways, and although many studies have demonstrated that Hsp90 regulates NF-¥êB activity, the exact mechanism is unclear. In this study, we investigated the relationship between Hsp90 and IKK¥ã in the regulation of NF-¥êB using expression plasmids of IKK complex components. Wild-type and deletion mutants of IKK¥ã were expressed together with Hsp90, and the combined regulatory effect of Hsp90 and IKK¥ã on NF-¥êB activation was assayed. The results show that Hsp90 activates NF-¥êB by promoting the phosphorylation and degradation of I¥êB¥á and that activation of NF-¥êB by NIK and LPS was increased by Hsp90. IKK¥ã elevated the effect of Hsp90 on NF-¥êB activation by increasing phosphorylation and degradation of I¥êB¥á. The positive regulation on NF-¥êB by Hsp90 and IKK¥ã was also proved in analysis with IKK¥â-EE, the constitutively active form of IKK¥â. In experiments with the deletion mutants of IKK¥ã, the N-terminal IKK¥â binding domain, C-terminal leucine zipper, and zinc finger domains of IKK¥ã were found not necessary for the positive regulation of NF-¥êB activity. Additionally, the expression of pro-inflammatory cytokines was synergistically elevated by Hsp90 and IKK¥ã. These results indicate that inhibiting the interaction between Hsp90 and IKK¥ã is a possible strategic method for controlling NF-¥êB and related diseases.
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KEYWORD
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Hsp90, inflammation, IKK¥â, IKK¥ã, NF-¥êB
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