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Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats

We analyzed the effect of diosgenin, administered with atorvastatin or ezetimibe, on the fate of (3)H(G)-taurocholic acid or 26-(14)C-cholesterol in hypercholesterolemic rats. Male Wistar rats received a hypercholesterolemic diet (HD), HD + atorvastatin (HD+ATV), HD + ezetimibe (HD+EZT), HD + diosge...

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Autores principales: Marín-Medina, Alejandro, Ruíz-Hidalgo, Gonzalo, Blé-Castillo, Jorge L., Zetina-Esquivel, Alma M., Zamora, Rodrigo Miranda, Juárez-Rojop, Isela E., Díaz-Zagoya, Juan C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6406618/
https://www.ncbi.nlm.nih.gov/pubmed/30791676
http://dx.doi.org/10.3390/ijerph16040627
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author Marín-Medina, Alejandro
Ruíz-Hidalgo, Gonzalo
Blé-Castillo, Jorge L.
Zetina-Esquivel, Alma M.
Zamora, Rodrigo Miranda
Juárez-Rojop, Isela E.
Díaz-Zagoya, Juan C.
author_facet Marín-Medina, Alejandro
Ruíz-Hidalgo, Gonzalo
Blé-Castillo, Jorge L.
Zetina-Esquivel, Alma M.
Zamora, Rodrigo Miranda
Juárez-Rojop, Isela E.
Díaz-Zagoya, Juan C.
author_sort Marín-Medina, Alejandro
collection PubMed
description We analyzed the effect of diosgenin, administered with atorvastatin or ezetimibe, on the fate of (3)H(G)-taurocholic acid or 26-(14)C-cholesterol in hypercholesterolemic rats. Male Wistar rats received a hypercholesterolemic diet (HD), HD + atorvastatin (HD+ATV), HD + ezetimibe (HD+EZT), HD + diosgenin (HD+DG), HD+ATV+EZT, or HD+ATV+DG for 40 days. We also included a control normal group (ND). The labelled compounds were administered on day 30. The animals were placed in metabolic cages for daily feces collection. At day 40 the rats were sacrificed. Lipid extracts from blood, liver, spinal cord, testicles, kidneys, epididymis, intestine, and feces were analyzed for radioactivity. Cholesterol activity was the highest in the liver in HD rats. DG diminished one half of this activity in HD+DG and HD+ATV+DG groups in comparison with the HD group. HD+ATV rats showed four to almost ten-fold cholesterol activity in the spinal cord compared with the ND or HD rats. Fecal elimination of neutral steroids was approximately two-fold higher in the HD+DG and HD+ATV+DG groups. Taurocholic acid activity was four to ten-fold higher in HD+DG intestine as compared to the other experimental groups. Taurocholic activity in the liver of HD and HD+DG groups was two and a half higher than in ND. Our results show that the combination of DG and ATV induced the highest cholesterol reduction in the liver and other tissues.
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spelling pubmed-64066182019-03-21 Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats Marín-Medina, Alejandro Ruíz-Hidalgo, Gonzalo Blé-Castillo, Jorge L. Zetina-Esquivel, Alma M. Zamora, Rodrigo Miranda Juárez-Rojop, Isela E. Díaz-Zagoya, Juan C. Int J Environ Res Public Health Article We analyzed the effect of diosgenin, administered with atorvastatin or ezetimibe, on the fate of (3)H(G)-taurocholic acid or 26-(14)C-cholesterol in hypercholesterolemic rats. Male Wistar rats received a hypercholesterolemic diet (HD), HD + atorvastatin (HD+ATV), HD + ezetimibe (HD+EZT), HD + diosgenin (HD+DG), HD+ATV+EZT, or HD+ATV+DG for 40 days. We also included a control normal group (ND). The labelled compounds were administered on day 30. The animals were placed in metabolic cages for daily feces collection. At day 40 the rats were sacrificed. Lipid extracts from blood, liver, spinal cord, testicles, kidneys, epididymis, intestine, and feces were analyzed for radioactivity. Cholesterol activity was the highest in the liver in HD rats. DG diminished one half of this activity in HD+DG and HD+ATV+DG groups in comparison with the HD group. HD+ATV rats showed four to almost ten-fold cholesterol activity in the spinal cord compared with the ND or HD rats. Fecal elimination of neutral steroids was approximately two-fold higher in the HD+DG and HD+ATV+DG groups. Taurocholic acid activity was four to ten-fold higher in HD+DG intestine as compared to the other experimental groups. Taurocholic activity in the liver of HD and HD+DG groups was two and a half higher than in ND. Our results show that the combination of DG and ATV induced the highest cholesterol reduction in the liver and other tissues. MDPI 2019-02-20 2019-02 /pmc/articles/PMC6406618/ /pubmed/30791676 http://dx.doi.org/10.3390/ijerph16040627 Text en © 2019 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
Marín-Medina, Alejandro
Ruíz-Hidalgo, Gonzalo
Blé-Castillo, Jorge L.
Zetina-Esquivel, Alma M.
Zamora, Rodrigo Miranda
Juárez-Rojop, Isela E.
Díaz-Zagoya, Juan C.
Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title_full Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title_fullStr Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title_full_unstemmed Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title_short Combined Effect of Diosgenin Along with Ezetimibe or Atorvastatin on the Fate of Labelled Bile Acid and Cholesterol in Hypercholesterolemic Rats
title_sort combined effect of diosgenin along with ezetimibe or atorvastatin on the fate of labelled bile acid and cholesterol in hypercholesterolemic rats
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6406618/
https://www.ncbi.nlm.nih.gov/pubmed/30791676
http://dx.doi.org/10.3390/ijerph16040627
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