Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification

End-stage renal disease is strongly associated with progressive cardiovascular calcification (CVC) and there is currently no therapy targeted to treat CVC. SNF472 is an experimental formulation under development for treatment of soft tissue calcification. We have investigated the pharmacokinetics of...

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Autores principales: Ferrer, Miguel D., Ketteler, Markus, Tur, Fernando, Tur, Eva, Isern, Bernat, Salcedo, Carolina, Joubert, Pieter H., Behets, Geert J., Neven, Ellen, D’Haese, Patrick C., Perelló, Joan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5942814/
https://www.ncbi.nlm.nih.gov/pubmed/29742152
http://dx.doi.org/10.1371/journal.pone.0197061
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author Ferrer, Miguel D.
Ketteler, Markus
Tur, Fernando
Tur, Eva
Isern, Bernat
Salcedo, Carolina
Joubert, Pieter H.
Behets, Geert J.
Neven, Ellen
D’Haese, Patrick C.
Perelló, Joan
author_facet Ferrer, Miguel D.
Ketteler, Markus
Tur, Fernando
Tur, Eva
Isern, Bernat
Salcedo, Carolina
Joubert, Pieter H.
Behets, Geert J.
Neven, Ellen
D’Haese, Patrick C.
Perelló, Joan
author_sort Ferrer, Miguel D.
collection PubMed
description End-stage renal disease is strongly associated with progressive cardiovascular calcification (CVC) and there is currently no therapy targeted to treat CVC. SNF472 is an experimental formulation under development for treatment of soft tissue calcification. We have investigated the pharmacokinetics of SNF472 administration in rats and its inhibitory effects on CVC. SNF472 was studied in three rat models: (1) prevention of vitamin D(3)-induced CVC with an intravenous SNF472 bolus of 1 mg/kg SNF472, (2) inhibition of progression of vitamin D(3)-induced CVC with a subcutaneous SNF472 bolus of 10 or 60 mg/kg SNF472, starting after calcification induction, (3) CVC in adenine-induced uremic rats treated with 50 mg/kg SNF472 via i.v. 4h -infusion. Uremic rats presented lower plasma levels of SNF472 than control animals after i.v. infusion. CVC in non-uremic rats was inhibited by 60–70% after treatment with SNF472 and progression of cardiac calcification completely blocked. Development of CVC in uremic rats was inhibited by up to 80% following i.v. infusion of SNF472. SNF472 inhibits the development and progression of CVC in uremic and non-uremic rats in the same range of SNF472 plasma levels but using in each case the required dose to obtain those levels. These results collectively support the development of SNF472 as a novel therapeutic option for treatment of CVC in humans.
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spelling pubmed-59428142018-05-18 Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification Ferrer, Miguel D. Ketteler, Markus Tur, Fernando Tur, Eva Isern, Bernat Salcedo, Carolina Joubert, Pieter H. Behets, Geert J. Neven, Ellen D’Haese, Patrick C. Perelló, Joan PLoS One Research Article End-stage renal disease is strongly associated with progressive cardiovascular calcification (CVC) and there is currently no therapy targeted to treat CVC. SNF472 is an experimental formulation under development for treatment of soft tissue calcification. We have investigated the pharmacokinetics of SNF472 administration in rats and its inhibitory effects on CVC. SNF472 was studied in three rat models: (1) prevention of vitamin D(3)-induced CVC with an intravenous SNF472 bolus of 1 mg/kg SNF472, (2) inhibition of progression of vitamin D(3)-induced CVC with a subcutaneous SNF472 bolus of 10 or 60 mg/kg SNF472, starting after calcification induction, (3) CVC in adenine-induced uremic rats treated with 50 mg/kg SNF472 via i.v. 4h -infusion. Uremic rats presented lower plasma levels of SNF472 than control animals after i.v. infusion. CVC in non-uremic rats was inhibited by 60–70% after treatment with SNF472 and progression of cardiac calcification completely blocked. Development of CVC in uremic rats was inhibited by up to 80% following i.v. infusion of SNF472. SNF472 inhibits the development and progression of CVC in uremic and non-uremic rats in the same range of SNF472 plasma levels but using in each case the required dose to obtain those levels. These results collectively support the development of SNF472 as a novel therapeutic option for treatment of CVC in humans. Public Library of Science 2018-05-09 /pmc/articles/PMC5942814/ /pubmed/29742152 http://dx.doi.org/10.1371/journal.pone.0197061 Text en © 2018 Ferrer et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Ferrer, Miguel D.
Ketteler, Markus
Tur, Fernando
Tur, Eva
Isern, Bernat
Salcedo, Carolina
Joubert, Pieter H.
Behets, Geert J.
Neven, Ellen
D’Haese, Patrick C.
Perelló, Joan
Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title_full Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title_fullStr Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title_full_unstemmed Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title_short Characterization of SNF472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
title_sort characterization of snf472 pharmacokinetics and efficacy in uremic and non-uremic rats models of cardiovascular calcification
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5942814/
https://www.ncbi.nlm.nih.gov/pubmed/29742152
http://dx.doi.org/10.1371/journal.pone.0197061
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