Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism

HDMX and its homologue HDM2 are two essential proteins for the cell; after genotoxic stress, both are phosphorylated near to their RING domain, specifically at serine 403 and 395, respectively. Once phosphorylated, both can bind the p53 mRNA and enhance its translation; however, both recognize p53 p...

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Autores principales: Calderon-González, Karla Gisel, Medina-Medina, Ixaura, Haronikova, Lucia, Hernychova, Lenka, Bonczek, Ondrej, Uhrik, Lukas, Hrabal, Vaclav, Vojtesek, Borivoj, Fahraeus, Robin, Hernández-Monge, Jesús, Olivares-Illana, Vanesa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Portland Press Ltd. 2022
Materias:
Biophysics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9254666/
https://www.ncbi.nlm.nih.gov/pubmed/35674210
http://dx.doi.org/10.1042/BSR20220186
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author Calderon-González, Karla Gisel
Medina-Medina, Ixaura
Haronikova, Lucia
Hernychova, Lenka
Bonczek, Ondrej
Uhrik, Lukas
Hrabal, Vaclav
Vojtesek, Borivoj
Fahraeus, Robin
Hernández-Monge, Jesús
Olivares-Illana, Vanesa
author_facet Calderon-González, Karla Gisel
Medina-Medina, Ixaura
Haronikova, Lucia
Hernychova, Lenka
Bonczek, Ondrej
Uhrik, Lukas
Hrabal, Vaclav
Vojtesek, Borivoj
Fahraeus, Robin
Hernández-Monge, Jesús
Olivares-Illana, Vanesa
author_sort Calderon-González, Karla Gisel
collection PubMed
description HDMX and its homologue HDM2 are two essential proteins for the cell; after genotoxic stress, both are phosphorylated near to their RING domain, specifically at serine 403 and 395, respectively. Once phosphorylated, both can bind the p53 mRNA and enhance its translation; however, both recognize p53 protein and provoke its degradation under normal conditions. HDM2 has been well-recognized as an E3 ubiquitin ligase, whereas it has been reported that even with the high similarity between the RING domains of the two homologs, HDMX does not have the E3 ligase activity. Despite this, HDMX is needed for the proper p53 poly-ubiquitination. Phosphorylation at serine 395 changes the conformation of HDM2, helping to explain the switch in its activity, but no information on HDMX has been published. Here, we study the conformation of HDMX and its phospho-mimetic mutant S403D, investigate its E3 ligase activity and dissect its binding with p53. We show that phospho-mutation does not change the conformation of the protein, but HDMX is indeed an E3 ubiquitin ligase in vitro; however, in vivo, no activity was found. We speculated that HDMX is regulated by induced fit, being able to switch activity accordingly to the specific partner as p53 protein, p53 mRNA or HDM2. Our results aim to contribute to the elucidation of the contribution of the HDMX to p53 regulation.
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spelling pubmed-92546662022-07-11 Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism Calderon-González, Karla Gisel Medina-Medina, Ixaura Haronikova, Lucia Hernychova, Lenka Bonczek, Ondrej Uhrik, Lukas Hrabal, Vaclav Vojtesek, Borivoj Fahraeus, Robin Hernández-Monge, Jesús Olivares-Illana, Vanesa Biosci Rep Biophysics HDMX and its homologue HDM2 are two essential proteins for the cell; after genotoxic stress, both are phosphorylated near to their RING domain, specifically at serine 403 and 395, respectively. Once phosphorylated, both can bind the p53 mRNA and enhance its translation; however, both recognize p53 protein and provoke its degradation under normal conditions. HDM2 has been well-recognized as an E3 ubiquitin ligase, whereas it has been reported that even with the high similarity between the RING domains of the two homologs, HDMX does not have the E3 ligase activity. Despite this, HDMX is needed for the proper p53 poly-ubiquitination. Phosphorylation at serine 395 changes the conformation of HDM2, helping to explain the switch in its activity, but no information on HDMX has been published. Here, we study the conformation of HDMX and its phospho-mimetic mutant S403D, investigate its E3 ligase activity and dissect its binding with p53. We show that phospho-mutation does not change the conformation of the protein, but HDMX is indeed an E3 ubiquitin ligase in vitro; however, in vivo, no activity was found. We speculated that HDMX is regulated by induced fit, being able to switch activity accordingly to the specific partner as p53 protein, p53 mRNA or HDM2. Our results aim to contribute to the elucidation of the contribution of the HDMX to p53 regulation. Portland Press Ltd. 2022-07-04 /pmc/articles/PMC9254666/ /pubmed/35674210 http://dx.doi.org/10.1042/BSR20220186 Text en © 2022 The Author(s). https://creativecommons.org/licenses/by/4.0/This is an open access article published by Portland Press Limited on behalf of the Biochemical Society and distributed under the Creative Commons Attribution License 4.0 (CC BY) (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Biophysics
Calderon-González, Karla Gisel
Medina-Medina, Ixaura
Haronikova, Lucia
Hernychova, Lenka
Bonczek, Ondrej
Uhrik, Lukas
Hrabal, Vaclav
Vojtesek, Borivoj
Fahraeus, Robin
Hernández-Monge, Jesús
Olivares-Illana, Vanesa
Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title_full Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title_fullStr Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title_full_unstemmed Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title_short Cryptic in vitro ubiquitin ligase activity of HDMX towards p53 is probably regulated by an induced fit mechanism
title_sort cryptic in vitro ubiquitin ligase activity of hdmx towards p53 is probably regulated by an induced fit mechanism
topic Biophysics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9254666/
https://www.ncbi.nlm.nih.gov/pubmed/35674210
http://dx.doi.org/10.1042/BSR20220186
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