The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome

In previous studies we have shown that oral Ang-(1–7) has a beneficial therapeutic effect on cardiometabolic disturbances present in metabolic syndrome (MetS). Based on the fact that Ang-(1–7) acts through release of nitric oxide (NO), a new peptide, A-1317 was engineered adding the amino acid L-Arg...

Descripción completa

Detalles Bibliográficos
Autores principales: Barbosa, Maria Andréa, Barbosa, Claudiane Maria, Lima, Taynara Carolina, dos Santos, Robson Augusto Souza, Alzamora, Andréia Carvalho
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Pharmacology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7476374/
https://www.ncbi.nlm.nih.gov/pubmed/32982727
http://dx.doi.org/10.3389/fphar.2020.01263
_version_ 1783579693242384384
author Barbosa, Maria Andréa
Barbosa, Claudiane Maria
Lima, Taynara Carolina
dos Santos, Robson Augusto Souza
Alzamora, Andréia Carvalho
author_facet Barbosa, Maria Andréa
Barbosa, Claudiane Maria
Lima, Taynara Carolina
dos Santos, Robson Augusto Souza
Alzamora, Andréia Carvalho
author_sort Barbosa, Maria Andréa
collection PubMed
description In previous studies we have shown that oral Ang-(1–7) has a beneficial therapeutic effect on cardiometabolic disturbances present in metabolic syndrome (MetS). Based on the fact that Ang-(1–7) acts through release of nitric oxide (NO), a new peptide, A-1317 was engineered adding the amino acid L-Arginine, the NO precursor, to the N-terminal portion of the Ang-(1–7). Therefore, in a single molecule the substrate and the activator of NO are combined. In the present study, we evaluated the effect of A-1317 oral treatment on liver-glucose metabolism in MetS induced by high fat (HF) diet in rats. Rats were subjected to control (AIN-93M, CT) or HF diets for 15 weeks to induce MetS and treated with A-1317, Ang-(1–7) included into hydroxypropyl-β-cyclodextrin (HPβCD) or empty HPβCD (E), in the last 7 weeks. At the end of 15 weeks, hemodynamic, biometric, and biochemical parameters, redox process, and qRT-PCR gene expression of NO synthase and RAS components were evaluated in the liver. HF/E rats increased body mass gain, adiposity index, despite the reduction in food intake, increased plasma leptin, total cholesterol, triglycerides, ALT, fasting blood glucose, OGTT and insulin, HOMA-IR and MAP and HR. Furthermore, the MetS rats presented increased in liver angiotensinogen, AT1R, ACE mRNA gene expression and concentration of MDA and carbonylated protein. Both Ang-(1–7) and A-1317 oral treatment in MetS rats reverted most of these alterations. However, A-1317 was more efficient in reducing body mass gain, ALT, AST, total cholesterol, insulin, fasting blood glucose, ameliorating β cell capacity by increasing HOMA-β and QUICKI, whereas Ang-(1–7) reduced HOMA-β and QUICKI. In addition, Ang-(1–7) increased Mas and AKT liver mRNA gene expression, while A-1317 increased both Mas and MRGD and AMPK liver mRNA gene expression, suggesting a distinct pathway of action of Ang-(1–7) and A-1317 in MetS rats. Taken together, our data showed that treatment with A-1317 was able to ameliorate MetS disorders and suggested that this effect was mainly via MRGD via activation of AMPK and increasing β cell function.
format Online
Article
Text
id pubmed-7476374
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-74763742020-09-26 The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome Barbosa, Maria Andréa Barbosa, Claudiane Maria Lima, Taynara Carolina dos Santos, Robson Augusto Souza Alzamora, Andréia Carvalho Front Pharmacol Pharmacology In previous studies we have shown that oral Ang-(1–7) has a beneficial therapeutic effect on cardiometabolic disturbances present in metabolic syndrome (MetS). Based on the fact that Ang-(1–7) acts through release of nitric oxide (NO), a new peptide, A-1317 was engineered adding the amino acid L-Arginine, the NO precursor, to the N-terminal portion of the Ang-(1–7). Therefore, in a single molecule the substrate and the activator of NO are combined. In the present study, we evaluated the effect of A-1317 oral treatment on liver-glucose metabolism in MetS induced by high fat (HF) diet in rats. Rats were subjected to control (AIN-93M, CT) or HF diets for 15 weeks to induce MetS and treated with A-1317, Ang-(1–7) included into hydroxypropyl-β-cyclodextrin (HPβCD) or empty HPβCD (E), in the last 7 weeks. At the end of 15 weeks, hemodynamic, biometric, and biochemical parameters, redox process, and qRT-PCR gene expression of NO synthase and RAS components were evaluated in the liver. HF/E rats increased body mass gain, adiposity index, despite the reduction in food intake, increased plasma leptin, total cholesterol, triglycerides, ALT, fasting blood glucose, OGTT and insulin, HOMA-IR and MAP and HR. Furthermore, the MetS rats presented increased in liver angiotensinogen, AT1R, ACE mRNA gene expression and concentration of MDA and carbonylated protein. Both Ang-(1–7) and A-1317 oral treatment in MetS rats reverted most of these alterations. However, A-1317 was more efficient in reducing body mass gain, ALT, AST, total cholesterol, insulin, fasting blood glucose, ameliorating β cell capacity by increasing HOMA-β and QUICKI, whereas Ang-(1–7) reduced HOMA-β and QUICKI. In addition, Ang-(1–7) increased Mas and AKT liver mRNA gene expression, while A-1317 increased both Mas and MRGD and AMPK liver mRNA gene expression, suggesting a distinct pathway of action of Ang-(1–7) and A-1317 in MetS rats. Taken together, our data showed that treatment with A-1317 was able to ameliorate MetS disorders and suggested that this effect was mainly via MRGD via activation of AMPK and increasing β cell function. Frontiers Media S.A. 2020-08-24 /pmc/articles/PMC7476374/ /pubmed/32982727 http://dx.doi.org/10.3389/fphar.2020.01263 Text en Copyright © 2020 Barbosa, Barbosa, Lima, Santos and Alzamora http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Barbosa, Maria Andréa
Barbosa, Claudiane Maria
Lima, Taynara Carolina
dos Santos, Robson Augusto Souza
Alzamora, Andréia Carvalho
The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title_full The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title_fullStr The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title_full_unstemmed The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title_short The Novel Angiotensin-(1–7) Analog, A-1317, Improves Insulin Resistance by Restoring Pancreatic β-Cell Functionality in Rats With Metabolic Syndrome
title_sort novel angiotensin-(1–7) analog, a-1317, improves insulin resistance by restoring pancreatic β-cell functionality in rats with metabolic syndrome
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7476374/
https://www.ncbi.nlm.nih.gov/pubmed/32982727
http://dx.doi.org/10.3389/fphar.2020.01263
work_keys_str_mv AT barbosamariaandrea thenovelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT barbosaclaudianemaria thenovelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT limataynaracarolina thenovelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT dossantosrobsonaugustosouza thenovelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT alzamoraandreiacarvalho thenovelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT barbosamariaandrea novelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT barbosaclaudianemaria novelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT limataynaracarolina novelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT dossantosrobsonaugustosouza novelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome
AT alzamoraandreiacarvalho novelangiotensin17analoga1317improvesinsulinresistancebyrestoringpancreaticbcellfunctionalityinratswithmetabolicsyndrome

Ejemplares similares