UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation

BACKGROUND: The proteins from the UBA-UBX family interact with ubiquitylated proteins via their UBA domain and with p97 via their UBX domain, thereby acting as substrate-binding adaptors for the p97 ATPase. In particular, human UBXN7 (also known as UBXD7) mediates p97 interaction with the transcript...

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Autores principales: Bandau, Susanne, Knebel, Axel, Gage, Zoe O, Wood, Nicola T, Alexandru, Gabriela
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3349548/
https://www.ncbi.nlm.nih.gov/pubmed/22537386
http://dx.doi.org/10.1186/1741-7007-10-36
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author Bandau, Susanne
Knebel, Axel
Gage, Zoe O
Wood, Nicola T
Alexandru, Gabriela
author_facet Bandau, Susanne
Knebel, Axel
Gage, Zoe O
Wood, Nicola T
Alexandru, Gabriela
author_sort Bandau, Susanne
collection PubMed
description BACKGROUND: The proteins from the UBA-UBX family interact with ubiquitylated proteins via their UBA domain and with p97 via their UBX domain, thereby acting as substrate-binding adaptors for the p97 ATPase. In particular, human UBXN7 (also known as UBXD7) mediates p97 interaction with the transcription factor HIF1α that is actively ubiquitylated in normoxic cells by a CUL2-based E3 ligase, CRL2. Mass spectrometry analysis of UBA-UBX protein immunoprecipitates showed that they interact with a multitude of E3 ubiquitin-ligases. Conspicuously, UBXN7 was most proficient in interacting with cullin-RING ligase subunits. We therefore set out to determine whether UBXN7 interaction with cullins was direct or mediated by its ubiquitylated targets bound to the UBA domain. RESULTS: We show that UBXN7 interaction with cullins is independent of ubiquitin- and substrate-binding. Instead, it relies on the UIM motif in UBXN7 that directly engages the NEDD8 modification on cullins. To understand the functional consequences of UBXN7 interaction with neddylated cullins, we focused on HIF1α, a CUL2 substrate that uses UBXD7/p97 as a ubiquitin-receptor on its way to proteasome-mediated degradation. We find that UBXN7 over-expression converts CUL2 to its neddylated form and causes the accumulation of non-ubiquitylated HIF1α. Both of these effects are strictly UIM-dependent and occur only when UBXN7 contains an intact UIM motif. We also show that HIF1α carrying long ubiquitin-chains can recruit alternative ubiquitin-receptors, lacking p97's ATP-dependent segregase activity. CONCLUSIONS: Our study shows that independently of its function as a ubiquitin-binding adaptor for p97, UBXN7 directly interacts with neddylated cullins and causes the accumulation of the CUL2 substrate HIF1α. We propose that by sequestering CUL2 in its neddylated form, UBXN7 negatively regulates the ubiquitin-ligase activity of CRL2 and this might prevent recruitment of ubiquitin-receptors other than p97 to nuclear HIF1α.
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spelling pubmed-33495482012-05-11 UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation Bandau, Susanne Knebel, Axel Gage, Zoe O Wood, Nicola T Alexandru, Gabriela BMC Biol Research Article BACKGROUND: The proteins from the UBA-UBX family interact with ubiquitylated proteins via their UBA domain and with p97 via their UBX domain, thereby acting as substrate-binding adaptors for the p97 ATPase. In particular, human UBXN7 (also known as UBXD7) mediates p97 interaction with the transcription factor HIF1α that is actively ubiquitylated in normoxic cells by a CUL2-based E3 ligase, CRL2. Mass spectrometry analysis of UBA-UBX protein immunoprecipitates showed that they interact with a multitude of E3 ubiquitin-ligases. Conspicuously, UBXN7 was most proficient in interacting with cullin-RING ligase subunits. We therefore set out to determine whether UBXN7 interaction with cullins was direct or mediated by its ubiquitylated targets bound to the UBA domain. RESULTS: We show that UBXN7 interaction with cullins is independent of ubiquitin- and substrate-binding. Instead, it relies on the UIM motif in UBXN7 that directly engages the NEDD8 modification on cullins. To understand the functional consequences of UBXN7 interaction with neddylated cullins, we focused on HIF1α, a CUL2 substrate that uses UBXD7/p97 as a ubiquitin-receptor on its way to proteasome-mediated degradation. We find that UBXN7 over-expression converts CUL2 to its neddylated form and causes the accumulation of non-ubiquitylated HIF1α. Both of these effects are strictly UIM-dependent and occur only when UBXN7 contains an intact UIM motif. We also show that HIF1α carrying long ubiquitin-chains can recruit alternative ubiquitin-receptors, lacking p97's ATP-dependent segregase activity. CONCLUSIONS: Our study shows that independently of its function as a ubiquitin-binding adaptor for p97, UBXN7 directly interacts with neddylated cullins and causes the accumulation of the CUL2 substrate HIF1α. We propose that by sequestering CUL2 in its neddylated form, UBXN7 negatively regulates the ubiquitin-ligase activity of CRL2 and this might prevent recruitment of ubiquitin-receptors other than p97 to nuclear HIF1α. BioMed Central 2012-04-26 /pmc/articles/PMC3349548/ /pubmed/22537386 http://dx.doi.org/10.1186/1741-7007-10-36 Text en Copyright ©2012 Bandau et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Bandau, Susanne
Knebel, Axel
Gage, Zoe O
Wood, Nicola T
Alexandru, Gabriela
UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title_full UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title_fullStr UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title_full_unstemmed UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title_short UBXN7 docks on neddylated cullin complexes using its UIM motif and causes HIF1α accumulation
title_sort ubxn7 docks on neddylated cullin complexes using its uim motif and causes hif1α accumulation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3349548/
https://www.ncbi.nlm.nih.gov/pubmed/22537386
http://dx.doi.org/10.1186/1741-7007-10-36
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