Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice

Takeda G protein-coupled receptor 5 (TGR5) agonists induce systemic release of glucagon-like peptides (GLPs) from intestinal L cells, a potentially therapeutic action against metabolic diseases such as nonalcoholic steatohepatitis (NASH), nonalcoholic fatty liver disease (NAFLD), and Type 2 diabetes...

Descripción completa

Detalles Bibliográficos
Autores principales: Finn, Patricia D., Rodriguez, David, Kohler, Jill, Jiang, Zhengfeng, Wan, Sindy, Blanco, Erick, King, Andrew J., Chen, Tao, Bell, Noah, Dragoli, Dean, Jacobs, Jeffrey W., Jain, Rakesh, Leadbetter, Michael, Siegel, Matthew, Carreras, Christopher W., Koo-McCoy, Samantha, Shaw, Karen, Le, Cathy, Vanegas, Sandra, Hsu, I-Hsin, Kozuka, Kenji, Okamoto, Keiko, Caldwell, Jeremy S., Lewis, Jason G.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Physiological Society 2019
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6459286/
https://www.ncbi.nlm.nih.gov/pubmed/30605011
http://dx.doi.org/10.1152/ajpgi.00300.2018
_version_ 1783410160099655680
author Finn, Patricia D.
Rodriguez, David
Kohler, Jill
Jiang, Zhengfeng
Wan, Sindy
Blanco, Erick
King, Andrew J.
Chen, Tao
Bell, Noah
Dragoli, Dean
Jacobs, Jeffrey W.
Jain, Rakesh
Leadbetter, Michael
Siegel, Matthew
Carreras, Christopher W.
Koo-McCoy, Samantha
Shaw, Karen
Le, Cathy
Vanegas, Sandra
Hsu, I-Hsin
Kozuka, Kenji
Okamoto, Keiko
Caldwell, Jeremy S.
Lewis, Jason G.
author_facet Finn, Patricia D.
Rodriguez, David
Kohler, Jill
Jiang, Zhengfeng
Wan, Sindy
Blanco, Erick
King, Andrew J.
Chen, Tao
Bell, Noah
Dragoli, Dean
Jacobs, Jeffrey W.
Jain, Rakesh
Leadbetter, Michael
Siegel, Matthew
Carreras, Christopher W.
Koo-McCoy, Samantha
Shaw, Karen
Le, Cathy
Vanegas, Sandra
Hsu, I-Hsin
Kozuka, Kenji
Okamoto, Keiko
Caldwell, Jeremy S.
Lewis, Jason G.
author_sort Finn, Patricia D.
collection PubMed
description Takeda G protein-coupled receptor 5 (TGR5) agonists induce systemic release of glucagon-like peptides (GLPs) from intestinal L cells, a potentially therapeutic action against metabolic diseases such as nonalcoholic steatohepatitis (NASH), nonalcoholic fatty liver disease (NAFLD), and Type 2 diabetes. Historically, TGR5 agonist use has been hindered by side effects, including inhibition of gallbladder emptying. Here, we characterize RDX8940, a novel, orally administered TGR5 agonist designed to have minimal systemic effects and investigate its activity in mice fed a Western diet, a model of NAFLD and mild insulin resistance. Agonist activity, binding selectivity, toxicity, solubility, and permeability of RDX8940 were characterized in standard in vitro models. RDX8940 pharmacokinetics and effects on GLP secretion, insulin sensitivity, and liver steatosis were assessed in C57BL/6 mice fed normal or Western diet chow and given single or repeated doses of RDX8940 or vehicle, with or without dipeptidyl peptidase-4 (DPP4) inhibitors. Gallbladder effects were assessed in CD-1 mice fed normal chow and given RDX8940 or a systemic TGR5 agonist or vehicle. Our results showed that RDX8940 is minimally systemic, potent, and selective, and induces incretin (GLP-1, GLP-2, and peptide YY) secretion. RDX8940-induced increases in plasma active GLP-1 (aGLP-1) levels were enhanced by repeated dosing and by coadministration of DPP4 inhibitors. RDX8940 increased hepatic exposure to aGLP-1 without requiring coadministration of a DPP4 inhibitor. In mice fed a Western diet, RDX8940 improved liver steatosis and insulin sensitivity. Unlike systemic TGR5 agonists, RDX8940 did not inhibit gallbladder emptying. These results indicate that RDX8940 may have therapeutic potential in patients with NAFLD/NASH. NEW & NOTEWORTHY Takeda G protein-coupled receptor 5 (TGR5) agonists have potential as a treatment for nonalcoholic steatohepatitis and nonalcoholic fatty liver disease (NAFLD) but have until now been associated with undesirable side effects associated with systemic TGR5 agonism, including blockade of gallbladder emptying. We demonstrate that RDX8940, a potent, selective, minimally systemic oral TGR5 agonist, improves liver steatosis and insulin sensitivity in a mouse model of NAFLD and does not inhibit gallbladder emptying in mice.
format Online
Article
Text
id pubmed-6459286
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher American Physiological Society
record_format MEDLINE/PubMed
spelling pubmed-64592862019-04-16 Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice Finn, Patricia D. Rodriguez, David Kohler, Jill Jiang, Zhengfeng Wan, Sindy Blanco, Erick King, Andrew J. Chen, Tao Bell, Noah Dragoli, Dean Jacobs, Jeffrey W. Jain, Rakesh Leadbetter, Michael Siegel, Matthew Carreras, Christopher W. Koo-McCoy, Samantha Shaw, Karen Le, Cathy Vanegas, Sandra Hsu, I-Hsin Kozuka, Kenji Okamoto, Keiko Caldwell, Jeremy S. Lewis, Jason G. Am J Physiol Gastrointest Liver Physiol Research Article Takeda G protein-coupled receptor 5 (TGR5) agonists induce systemic release of glucagon-like peptides (GLPs) from intestinal L cells, a potentially therapeutic action against metabolic diseases such as nonalcoholic steatohepatitis (NASH), nonalcoholic fatty liver disease (NAFLD), and Type 2 diabetes. Historically, TGR5 agonist use has been hindered by side effects, including inhibition of gallbladder emptying. Here, we characterize RDX8940, a novel, orally administered TGR5 agonist designed to have minimal systemic effects and investigate its activity in mice fed a Western diet, a model of NAFLD and mild insulin resistance. Agonist activity, binding selectivity, toxicity, solubility, and permeability of RDX8940 were characterized in standard in vitro models. RDX8940 pharmacokinetics and effects on GLP secretion, insulin sensitivity, and liver steatosis were assessed in C57BL/6 mice fed normal or Western diet chow and given single or repeated doses of RDX8940 or vehicle, with or without dipeptidyl peptidase-4 (DPP4) inhibitors. Gallbladder effects were assessed in CD-1 mice fed normal chow and given RDX8940 or a systemic TGR5 agonist or vehicle. Our results showed that RDX8940 is minimally systemic, potent, and selective, and induces incretin (GLP-1, GLP-2, and peptide YY) secretion. RDX8940-induced increases in plasma active GLP-1 (aGLP-1) levels were enhanced by repeated dosing and by coadministration of DPP4 inhibitors. RDX8940 increased hepatic exposure to aGLP-1 without requiring coadministration of a DPP4 inhibitor. In mice fed a Western diet, RDX8940 improved liver steatosis and insulin sensitivity. Unlike systemic TGR5 agonists, RDX8940 did not inhibit gallbladder emptying. These results indicate that RDX8940 may have therapeutic potential in patients with NAFLD/NASH. NEW & NOTEWORTHY Takeda G protein-coupled receptor 5 (TGR5) agonists have potential as a treatment for nonalcoholic steatohepatitis and nonalcoholic fatty liver disease (NAFLD) but have until now been associated with undesirable side effects associated with systemic TGR5 agonism, including blockade of gallbladder emptying. We demonstrate that RDX8940, a potent, selective, minimally systemic oral TGR5 agonist, improves liver steatosis and insulin sensitivity in a mouse model of NAFLD and does not inhibit gallbladder emptying in mice. American Physiological Society 2019-03-01 2019-01-03 /pmc/articles/PMC6459286/ /pubmed/30605011 http://dx.doi.org/10.1152/ajpgi.00300.2018 Text en Copyright © 2019 the American Physiological Society http://creativecommons.org/licenses/by/4.0/deed.en_US Licensed under Creative Commons Attribution CC-BY 4.0 (http://creativecommons.org/licenses/by/4.0/deed.en_US) : © the American Physiological Society.
spellingShingle Research Article
Finn, Patricia D.
Rodriguez, David
Kohler, Jill
Jiang, Zhengfeng
Wan, Sindy
Blanco, Erick
King, Andrew J.
Chen, Tao
Bell, Noah
Dragoli, Dean
Jacobs, Jeffrey W.
Jain, Rakesh
Leadbetter, Michael
Siegel, Matthew
Carreras, Christopher W.
Koo-McCoy, Samantha
Shaw, Karen
Le, Cathy
Vanegas, Sandra
Hsu, I-Hsin
Kozuka, Kenji
Okamoto, Keiko
Caldwell, Jeremy S.
Lewis, Jason G.
Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title_full Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title_fullStr Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title_full_unstemmed Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title_short Intestinal TGR5 agonism improves hepatic steatosis and insulin sensitivity in Western diet-fed mice
title_sort intestinal tgr5 agonism improves hepatic steatosis and insulin sensitivity in western diet-fed mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6459286/
https://www.ncbi.nlm.nih.gov/pubmed/30605011
http://dx.doi.org/10.1152/ajpgi.00300.2018
work_keys_str_mv AT finnpatriciad intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT rodriguezdavid intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT kohlerjill intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT jiangzhengfeng intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT wansindy intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT blancoerick intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT kingandrewj intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT chentao intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT bellnoah intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT dragolidean intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT jacobsjeffreyw intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT jainrakesh intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT leadbettermichael intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT siegelmatthew intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT carreraschristopherw intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT koomccoysamantha intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT shawkaren intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT lecathy intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT vanegassandra intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT hsuihsin intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT kozukakenji intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT okamotokeiko intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT caldwelljeremys intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice
AT lewisjasong intestinaltgr5agonismimproveshepaticsteatosisandinsulinsensitivityinwesterndietfedmice

Ejemplares similares