Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes

BACKGROUND: The bile acid (BA) pathway plays a role in regulation of food intake and glucose metabolism, based mainly on findings in animal models. Our aim was to determine whether the BA pathway is altered and correctable in human obesity and diabetes. METHODS: We conducted 3 investigations: 1) BA...

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Autores principales: Calderon, Gerardo, McRae, Alison, Rievaj, Juraj, Davis, Judith, Zandvakili, Inuk, Linker-Nord, Sara, Burton, Duane, Roberts, Geoffrey, Reimann, Frank, Gedulin, Bronislava, Vella, Adrian, LaRusso, Nicholas F, Camilleri, Michael, Gribble, Fiona M, Acosta, Andres
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Research paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7186521/
https://www.ncbi.nlm.nih.gov/pubmed/32344198
http://dx.doi.org/10.1016/j.ebiom.2020.102759
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author Calderon, Gerardo
McRae, Alison
Rievaj, Juraj
Davis, Judith
Zandvakili, Inuk
Linker-Nord, Sara
Burton, Duane
Roberts, Geoffrey
Reimann, Frank
Gedulin, Bronislava
Vella, Adrian
LaRusso, Nicholas F
Camilleri, Michael
Gribble, Fiona M
Acosta, Andres
author_facet Calderon, Gerardo
McRae, Alison
Rievaj, Juraj
Davis, Judith
Zandvakili, Inuk
Linker-Nord, Sara
Burton, Duane
Roberts, Geoffrey
Reimann, Frank
Gedulin, Bronislava
Vella, Adrian
LaRusso, Nicholas F
Camilleri, Michael
Gribble, Fiona M
Acosta, Andres
author_sort Calderon, Gerardo
collection PubMed
description BACKGROUND: The bile acid (BA) pathway plays a role in regulation of food intake and glucose metabolism, based mainly on findings in animal models. Our aim was to determine whether the BA pathway is altered and correctable in human obesity and diabetes. METHODS: We conducted 3 investigations: 1) BA receptor pathways were studied in NCI-H716 enteroendocrine cell (EEC) line, whole human colonic mucosal tissue and in human colonic EEC isolated by Fluorescence-activated Cell Sorting (ex vivo) from endoscopically-obtained biopsies colon mucosa; 2) We characterized the BA pathway in 307 participants by measuring during fasting and postprandial levels of FGF19, 7αC4 and serum BA; 3) In a placebo-controlled, double-blind, randomised, 28-day trial, we studied the effect of ileo-colonic delivery of conjugated BAs (IC-CBAS) on glucose metabolism, incretins, and lipids, in participants with obesity and diabetes. FINDINGS: Human colonic GLP-1-producing EECs express TGR5, and upon treatment with bile acids in vitro, human EEC differentially expressed GLP-1 at the protein and mRNA level. In Ussing Chamber, GLP-1 release was stimulated by Taurocholic acid in either the apical or basolateral compartment. FGF19 was decreased in obesity and diabetes compared to controls. When compared to placebo, IC-CBAS significantly decreased postprandial glucose, fructosamine, fasting insulin, fasting LDL, and postprandial FGF19 and increased postprandial GLP-1 and C-peptide. Increase in faecal BA was associated with weight loss and with decreased fructosamine. INTERPRETATIONS: In humans, BA signalling machinery is expressed in colonic EECs, deficient in obesity and diabetes, and when stimulated with IC-CBAS, improved glucose homeostasis. ClinicalTrials.gov number, NCT02871882, NCT02033876. FUNDING: Research support and drug was provided by Satiogen Pharmaceuticals (San Diego, CA). AA, MC, and NFL report grants (AA- C-Sig P30DK84567, K23 DK114460; MC- NIH R01 DK67071; NFL- R01 DK057993) from the NIH. JR was supported by an Early Career Grant from Society for Endocrinology.
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spelling pubmed-71865212020-05-04 Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes Calderon, Gerardo McRae, Alison Rievaj, Juraj Davis, Judith Zandvakili, Inuk Linker-Nord, Sara Burton, Duane Roberts, Geoffrey Reimann, Frank Gedulin, Bronislava Vella, Adrian LaRusso, Nicholas F Camilleri, Michael Gribble, Fiona M Acosta, Andres EBioMedicine Research paper BACKGROUND: The bile acid (BA) pathway plays a role in regulation of food intake and glucose metabolism, based mainly on findings in animal models. Our aim was to determine whether the BA pathway is altered and correctable in human obesity and diabetes. METHODS: We conducted 3 investigations: 1) BA receptor pathways were studied in NCI-H716 enteroendocrine cell (EEC) line, whole human colonic mucosal tissue and in human colonic EEC isolated by Fluorescence-activated Cell Sorting (ex vivo) from endoscopically-obtained biopsies colon mucosa; 2) We characterized the BA pathway in 307 participants by measuring during fasting and postprandial levels of FGF19, 7αC4 and serum BA; 3) In a placebo-controlled, double-blind, randomised, 28-day trial, we studied the effect of ileo-colonic delivery of conjugated BAs (IC-CBAS) on glucose metabolism, incretins, and lipids, in participants with obesity and diabetes. FINDINGS: Human colonic GLP-1-producing EECs express TGR5, and upon treatment with bile acids in vitro, human EEC differentially expressed GLP-1 at the protein and mRNA level. In Ussing Chamber, GLP-1 release was stimulated by Taurocholic acid in either the apical or basolateral compartment. FGF19 was decreased in obesity and diabetes compared to controls. When compared to placebo, IC-CBAS significantly decreased postprandial glucose, fructosamine, fasting insulin, fasting LDL, and postprandial FGF19 and increased postprandial GLP-1 and C-peptide. Increase in faecal BA was associated with weight loss and with decreased fructosamine. INTERPRETATIONS: In humans, BA signalling machinery is expressed in colonic EECs, deficient in obesity and diabetes, and when stimulated with IC-CBAS, improved glucose homeostasis. ClinicalTrials.gov number, NCT02871882, NCT02033876. FUNDING: Research support and drug was provided by Satiogen Pharmaceuticals (San Diego, CA). AA, MC, and NFL report grants (AA- C-Sig P30DK84567, K23 DK114460; MC- NIH R01 DK67071; NFL- R01 DK057993) from the NIH. JR was supported by an Early Career Grant from Society for Endocrinology. Elsevier 2020-04-25 /pmc/articles/PMC7186521/ /pubmed/32344198 http://dx.doi.org/10.1016/j.ebiom.2020.102759 Text en © 2020 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research paper
Calderon, Gerardo
McRae, Alison
Rievaj, Juraj
Davis, Judith
Zandvakili, Inuk
Linker-Nord, Sara
Burton, Duane
Roberts, Geoffrey
Reimann, Frank
Gedulin, Bronislava
Vella, Adrian
LaRusso, Nicholas F
Camilleri, Michael
Gribble, Fiona M
Acosta, Andres
Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title_full Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title_fullStr Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title_full_unstemmed Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title_short Ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic GLP-1-producing enteroendocrine cells in human obesity and diabetes
title_sort ileo-colonic delivery of conjugated bile acids improves glucose homeostasis via colonic glp-1-producing enteroendocrine cells in human obesity and diabetes
topic Research paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7186521/
https://www.ncbi.nlm.nih.gov/pubmed/32344198
http://dx.doi.org/10.1016/j.ebiom.2020.102759
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