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KMID : 0923620190190030016
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Immune Network
2019 Volume.19 No. 3 p.16 ~ p.16
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p62 Negatively Regulates TLR4 Signaling via Functional Regulation of the TRAF6-ECSIT Complex
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Kim Mi-Jeong
Min Yoon
Kwon Jeong-Ho
Son Ju-Hee
Im Ji-Seon
Shin Jae-Kyoon
Lee Ki-Young
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Abstract
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Sequestosome 1 (SQSTM1, p62), a ubiquitin binding protein, plays a role in cell signaling, oxidative stress, and autophagy. However, its functional role in inflammatory signaling is controversial. Recent studies have shown that p62 is negatively implicated in inflammatory responses. But, the precise molecular mechanisms by which p62 regulates inflammatory responses remain unclear. In this study, we report on a new regulatory role for p62 in TLR4-mediated signaling. p62 overexpression led to the suppression of NF-¥êB activation and the production of pro-inflammatory cytokines, TNF-¥á, IL-6, and IL-1¥â in response to TLR4 stimulation. In contrast, p62?/? mouse embryonic fibroblast (MEF) cells exhibited marked enhancement of NF-¥êB activation and production of pro-inflammatory cytokines by TLR4 stimulation, compared to p62+/+ MEF cells. Additionally, the TLR4-induced activation of signal transduction was significantly augmented in p62?/? MEF cells, indicating that p62 was negatively implicated in TLR4-mediated signaling. Biochemical studies revealed that p62 interacted with the internal domain of evolutionarily conserved signaling intermediate in Toll pathways (ECSIT), which is critical for associating with the TNF receptor associated factor 6 (TRAF6)-ECSIT complex to activate NF-¥êB in TLR4 signaling. Interestingly, p62-ECSIT interaction inhibited the interaction between TRAF6 and ECSIT and attenuated the ubiquitination of ECSIT. Furthermore, upon LPS challenge, the mortality of p62?/? (p62-knockout) mice was markedly enhanced compared to p62+/+ (p62 wild-type) mice. Taken together, our data demonstrate that p62 negatively regulated TLR4 signaling via functional regulation of the TRAF6-ECSIT complex.
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KEYWORD
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Sequestosome 1, TLR4 receptor, TRAF6, ECSIT, NF-¥êB
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