A liver-targeting Cu(i) chelator relocates Cu in hepatocytes and promotes Cu excretion in a murine model of Wilson's disease.


Journal

Metallomics : integrated biometal science
ISSN: 1756-591X
Titre abrégé: Metallomics
Pays: England
ID NLM: 101478346

Informations de publication

Date de publication:
24 06 2020
Historique:
pubmed: 14 5 2020
medline: 10 8 2021
entrez: 14 5 2020
Statut: ppublish

Résumé

Copper chelation is the most commonly used therapeutic strategy nowadays to treat Wilson's disease, a genetic disorder primarily inducing a pathological accumulation of Cu in the liver. The mechanism of action of Chel2, a liver-targeting Cu(i) chelator known to promote intracellular Cu chelation, was studied in hepatic cells that reconstitute polarized epithelia with functional bile canaliculi, reminiscent of the excretion pathway in the liver. The interplay between Chel2 and Cu localization in these cells was demonstrated through confocal microscopy using a fluorescent derivative and nano X-ray fluorescence. The Cu(i) bound chelator was found in vesicles potentially excreted in the canaliculi. Moreover, injection of Chel2 either intravenously or subcutaneously to a murine model of Wilson's disease increased excretion of Cu in the faeces, confirming in vivo biliary excretion. Therefore, Chel2 turns out to be a possible means to collect and excrete hepatic Cu in the faeces, hence restoring the physiological pathway.

Identifiants

pubmed: 32401247
doi: 10.1039/d0mt00069h
doi:

Substances chimiques

Copper 789U1901C5
Ceruloplasmin EC 1.16.3.1

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

1000-1008

Auteurs

Marie Monestier (M)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France and Univ. Grenoble Alpes, CEA, CNRS, IRIG, SyMMES, F-38000 Grenoble, France. pascale.delangle@cea.fr.

Anaïs M Pujol (AM)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France and Univ. Grenoble Alpes, CEA, CNRS, IRIG, SyMMES, F-38000 Grenoble, France. pascale.delangle@cea.fr.

Aline Lamboux (A)

Univ. Lyon, CNRS, ENS de Lyon, LGLTPE, F-69007 Lyon, France.

Martine Cuillel (M)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France.

Isabelle Pignot-Paintrand (I)

Univ. Grenoble Alpes, CNRS, Grenoble INP, LMGP, F-38000 Grenoble, France.

Doris Cassio (D)

INSERM, Univ. Paris Sud, UMR U 1174, F-91405 Orsay, France.

Peggy Charbonnier (P)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France.

Khémary Um (K)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France.

Amélie Harel (A)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France.

Sylvain Bohic (S)

Inserm, UA7, Synchrotron Radiation for Biomedicine (STROBE), 38000, Grenoble, France.

Christelle Gateau (C)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, SyMMES, F-38000 Grenoble, France. pascale.delangle@cea.fr.

Vincent Balter (V)

Univ. Lyon, CNRS, ENS de Lyon, LGLTPE, F-69007 Lyon, France.

Virginie Brun (V)

Univ. Grenoble Alpes, CEA, INSERM, IRIG, BGE, F-38000 Grenoble, France.

Pascale Delangle (P)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, SyMMES, F-38000 Grenoble, France. pascale.delangle@cea.fr.

Elisabeth Mintz (E)

Univ. Grenoble Alpes, CEA, CNRS, IRIG, LCBM, F-38000 Grenoble, France.

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Classifications MeSH