An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population

The H1069Q substitution is the most frequent mutation of the Cu transporter ATP7B that causes Wilson disease in the Caucasian population. ATP7B localizes to the Golgi complex in hepatocytes, but, in the presence of excessive Cu, it relocates to the endo-lysosomal compartment to excrete Cu via bile c...

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Autores principales: Allocca, Simona, Ciano, Michela, Ciardulli, Maria Camilla, D’Ambrosio, Chiara, Scaloni, Andrea, Sarnataro, Daniela, Caporaso, Maria Gabriella, D’Agostino, Massimo, Bonatti, Stefano
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2018
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6073935/
https://www.ncbi.nlm.nih.gov/pubmed/29954118
http://dx.doi.org/10.3390/ijms19071892
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author Allocca, Simona
Ciano, Michela
Ciardulli, Maria Camilla
D’Ambrosio, Chiara
Scaloni, Andrea
Sarnataro, Daniela
Caporaso, Maria Gabriella
D’Agostino, Massimo
Bonatti, Stefano
author_facet Allocca, Simona
Ciano, Michela
Ciardulli, Maria Camilla
D’Ambrosio, Chiara
Scaloni, Andrea
Sarnataro, Daniela
Caporaso, Maria Gabriella
D’Agostino, Massimo
Bonatti, Stefano
author_sort Allocca, Simona
collection PubMed
description The H1069Q substitution is the most frequent mutation of the Cu transporter ATP7B that causes Wilson disease in the Caucasian population. ATP7B localizes to the Golgi complex in hepatocytes, but, in the presence of excessive Cu, it relocates to the endo-lysosomal compartment to excrete Cu via bile canaliculi. In contrast, ATP7B-H1069Q is strongly retained in the ER, does not reach the Golgi complex and fails to move to the endo-lysosomal compartment in the presence of excessive Cu, thus causing toxic Cu accumulation. We have previously shown that, in transfected cells, the small heat-shock protein αB-crystallin is able to correct the mislocalization of ATP7B-H1069Q and its trafficking in the presence of Cu overload. Here, we first show that the α-crystallin domain of αB-crystallin mimics the effect of the full-length protein, whereas the N- and C-terminal domains have no such effect. Next, and most importantly, we demonstrate that a twenty-residue peptide derived from the α-crystallin domain of αB-crystallin fully rescues Golgi localization and the trafficking response of ATP7B-H1069Q in the presence of Cu overload. In addition, we show that this peptide interacts with the mutant transporter in the live cell. These results open the way to attempt developing a pharmacologically active peptide to specifically contrast the Wilson disease form caused by the ATP7B-H1069Q mutant.
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spelling pubmed-60739352018-08-13 An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population Allocca, Simona Ciano, Michela Ciardulli, Maria Camilla D’Ambrosio, Chiara Scaloni, Andrea Sarnataro, Daniela Caporaso, Maria Gabriella D’Agostino, Massimo Bonatti, Stefano Int J Mol Sci Article The H1069Q substitution is the most frequent mutation of the Cu transporter ATP7B that causes Wilson disease in the Caucasian population. ATP7B localizes to the Golgi complex in hepatocytes, but, in the presence of excessive Cu, it relocates to the endo-lysosomal compartment to excrete Cu via bile canaliculi. In contrast, ATP7B-H1069Q is strongly retained in the ER, does not reach the Golgi complex and fails to move to the endo-lysosomal compartment in the presence of excessive Cu, thus causing toxic Cu accumulation. We have previously shown that, in transfected cells, the small heat-shock protein αB-crystallin is able to correct the mislocalization of ATP7B-H1069Q and its trafficking in the presence of Cu overload. Here, we first show that the α-crystallin domain of αB-crystallin mimics the effect of the full-length protein, whereas the N- and C-terminal domains have no such effect. Next, and most importantly, we demonstrate that a twenty-residue peptide derived from the α-crystallin domain of αB-crystallin fully rescues Golgi localization and the trafficking response of ATP7B-H1069Q in the presence of Cu overload. In addition, we show that this peptide interacts with the mutant transporter in the live cell. These results open the way to attempt developing a pharmacologically active peptide to specifically contrast the Wilson disease form caused by the ATP7B-H1069Q mutant. MDPI 2018-06-27 /pmc/articles/PMC6073935/ /pubmed/29954118 http://dx.doi.org/10.3390/ijms19071892 Text en © 2018 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Allocca, Simona
Ciano, Michela
Ciardulli, Maria Camilla
D’Ambrosio, Chiara
Scaloni, Andrea
Sarnataro, Daniela
Caporaso, Maria Gabriella
D’Agostino, Massimo
Bonatti, Stefano
An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title_full An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title_fullStr An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title_full_unstemmed An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title_short An αB-Crystallin Peptide Rescues Compartmentalization and Trafficking Response to Cu Overload of ATP7B-H1069Q, the Most Frequent Cause of Wilson Disease in the Caucasian Population
title_sort αb-crystallin peptide rescues compartmentalization and trafficking response to cu overload of atp7b-h1069q, the most frequent cause of wilson disease in the caucasian population
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6073935/
https://www.ncbi.nlm.nih.gov/pubmed/29954118
http://dx.doi.org/10.3390/ijms19071892
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