The p62 Scaffold Regulates Nerve Growth Factor-induced NF-κB Activation by Influencing TRAF6 Polyubiquitination

Wooten, Marie W.; Geetha, Thangiah; Seibenhener, M. Lamar; Babu, Jeganathan Ramesh; Diaz-Meco, Marı́a T.; Moscat, Jorge

doi:10.1074/jbc.c500237200

Cited by 201 publications

(222 citation statements)

References 33 publications

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“…The relative contribution at these two levels upstream and downstream of IKK and the physiological regulation of b-arrestins in NF-kB pathways are not yet fully explored. Finally, sequestosome 1/p62, a scaffolding protein that also binds to TRAF6 and facilitates TRAF6 oligomerization and Ub Lys63 modification has been shown to be required for the nerve growth factor-induced IKK/NF-kB pathway (Wooten et al, 2005).…”

Section: Ubiquitin-mediated Ikk Regulationmentioning

confidence: 99%

IκB kinase complexes: gateways to NF-κB activation and transcription

2006

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Section: Ubiquitin-mediated Ikk Regulationmentioning

confidence: 99%

IκB kinase complexes: gateways to NF-κB activation and transcription

2006

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“…Human embryonic kidney (HEK) 293 and nnr5 cells were grown as previously described [8]. HEK293 cells were transfected with the calcium phosphate method by using a Mammalian Cell Transfection Kit (Specialty Media), and nnr5 cells were transfected by using LipofectAMINE 2000 (Invitrogen Life Technologies).…”

Section: Cell Culturementioning

confidence: 99%

“…Moreover, it appears that the E3 targets an accessible surface residue providing the selection process with a conformational recognition mechanism. The TRAF6-p62 signaling complex leads to autoactivation of TRAF6 [8]. The scaffold, p62, then recruits the substrate enabling the E3 to scan for the easily accessible lysine residues in the loops and helical structures on the surface of the substrate resulting in polyubiquitination at a specific lysine, if the flanking residues fit the consensus motif.…”

Section: Receptor Ubiquitination Implicated In Regulation Of Trkb Dowmentioning

confidence: 99%

“…P62 serves as an adaptor bridge to recruit TRAF6 through its TRAF6 binding site [3,8,9]. Therefore, studies were undertaken to examine whether mutation at the primary ubiquitination site in the TrkB receptor impairs formation of a TRAF6/p62 signaling complex.…”

Section: Mutation Impairs P62's Ability To Link Trkb To Traf6mentioning

confidence: 99%

“…In this regard, p62 has been shown to act as an adaptor and interacts with the TRAF domain of TRAF6, resulting in its auto-activation [7,8]. Recent findings from our lab have revealed that both TrkA [9] and the neurotrophin receptor interacting factor (NRIF) [10] are K63-polyubiquitinated by the TRAF6/p62 complex.…”

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confidence: 99%

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Identification of a consensus site for TRAF6/p62 polyubiquitination

Jadhav

Geetha

Jiang

et al. 2008

Biochemical and Biophysical Research Communications

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Tumor necrosis factor receptor-associated factor 6 (TRAF6) is an ubiquitin ligase that regulates a diverse array of physiological processes via forming Lys-63 linked polyubiquitin chains. In this study, the lysine selection process for TRAF6/p62 ubiquitination was examined. The protein sequence of two characterized TRAF6/p62 substrates, NRIF and TrkA, revealed a conserved consensus pattern for the ubiquitination site of these two TRAF6 substrates. The consensus pattern established in the verified substrates was common to the other Trk receptor family members, TrkB and TrkC. Interestingly, Lysine 811 in TrkB was selected for ubiquination, and mutation of Lysine 811 diminished the formation of TRAF6/p62 complex that is necessary for effective ubiquination. Moreover, downstream signaling was affected upon binding of BDNF to the mutant TrkB receptor. These findings reveal a possible selection process for targeting a specific lysine residue by a single E3 ligase and underscore the role of the scaffold, p62, in this process. KeywordsUbiquitination; Ub ligase; TRAF6; p62; Trk Many adaptors have been identified in studies of other neuronal tyrosine kinases that may also prove to function in Trk receptor-mediated signaling [1]. Cytoplasmic protein p62 was identified as an interacting partner of atypical protein kinase C (PKC) [2] and has been shown to contain several protein-protein interacting modules that enable the protein to serve as a scaffold for activation of the transcription factor NF-κB [3]. The multidomain protein structure of p62 is suggestive of diverse protein-protein interactions and its link in cellular functions. The functional motifs in p62 include a Phox and Bem1p domain (PB1) domain that embeds an octicosapeptide Phox, Cdc and the atypical PKC-interaction domain (AID) (OPCA) motif, a ZZ zinc finger, a binding site for Tumor necrosis factor Receptor-Associated Factor 6 (TRAF6), two PEST sequences, and an Ubiquitin-associated (UBA) domain [4]. The Cterminal ubiquitin-associated domain (UBA) was discovered to bind non-covalently to ubiquitin [5]. In vitro binding studies have unveiled p62 as a unique ubiquitin-binding protein, which binds polyubiquitin non-covalently through its C-terminus [6].Ubiquitination of eukaryotic proteins regulates a broad range of cellular processes. E3 Ub ligases are known to interact with specific substrates either directly or through adaptor proteins. *Corresponding author. Fax: +1 (334) 844-5255, Email address: wootemw@auburn.edu (M. Wooten). Publisher's Disclaimer: This is a PDF file of an unedited manuscript that has been accepted for publication. As a service to our customers we are providing this early version of the manuscript. The manuscript will undergo copyediting, typesetting, and review of the resulting proof before it is published in its final citable form. Please note that during the production process errors may be discovered which could affect the content, and all legal disclaimers that apply to the journal pertain. . High substrate specificity of the ...

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p62/SQSTM1—Dr. Jekyll and Mr. Hyde that prevents oxidative stress but promotes liver cancer

Taniguchi

Yamachika

et al. 2016

FEBS Letters

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p62/SQSTM1 is a multifunctional signaling hub and autophagy adaptor with many binding partners, which allow it to activate mTORC1-dependent nutrient sensing, NF-κB-mediated inflammatory responses and the NRF2-activated antioxidant defense. p62 recognizes polyubiquitin chains via its C-terminal domain and binds to LC3 via its LIR motif, thereby promoting the autophagic degradation of ubiquitinated cargos. p62 accumulates in many human liver diseases, including non-alcoholic steatohepatitis (NASH) and hepatocellular carcinoma (HCC), where it is a component of Mallory-Denk bodies and intracellular hyaline bodies. Chronic p62 elevation contributes to HCC development by preventing oncogene-induced senescence and death of cancer-initiating cells and enhancing their proliferation. In this review, we discuss p62-mediated signaling pathways and their roles in liver pathophysiology, especially NASH and HCC.

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The p62 Scaffold Regulates Nerve Growth Factor-induced NF-κB Activation by Influencing TRAF6 Polyubiquitination

Cited by 201 publications

References 33 publications

IκB kinase complexes: gateways to NF-κB activation and transcription

IκB kinase complexes: gateways to NF-κB activation and transcription

Identification of a consensus site for TRAF6/p62 polyubiquitination

p62/SQSTM1—Dr. Jekyll and Mr. Hyde that prevents oxidative stress but promotes liver cancer

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