Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits

OBJECTIVES: Extracts of the hops plant have been shown to reduce weight and insulin resistance in rodents and humans, but elucidation of the mechanisms responsible for these benefits has been hindered by the use of heterogeneous hops-derived mixtures. Because hop extracts are used as flavoring agent...

Descripción completa

Detalles Bibliográficos
Autores principales: Kok, Bernard P., Galmozzi, Andrea, Littlejohn, Nicole K., Albert, Verena, Godio, Cristina, Kim, Woojoo, Kim, Sean M., Bland, Jeffrey S., Grayson, Neile, Fang, Mingliang, Meyerhof, Wolfgang, Siuzdak, Gary, Srinivasan, Supriya, Behrens, Maik, Saez, Enrique
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2018
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6158035/
https://www.ncbi.nlm.nih.gov/pubmed/30120064
http://dx.doi.org/10.1016/j.molmet.2018.07.013
_version_ 1783358365402923008
author Kok, Bernard P.
Galmozzi, Andrea
Littlejohn, Nicole K.
Albert, Verena
Godio, Cristina
Kim, Woojoo
Kim, Sean M.
Bland, Jeffrey S.
Grayson, Neile
Fang, Mingliang
Meyerhof, Wolfgang
Siuzdak, Gary
Srinivasan, Supriya
Behrens, Maik
Saez, Enrique
author_facet Kok, Bernard P.
Galmozzi, Andrea
Littlejohn, Nicole K.
Albert, Verena
Godio, Cristina
Kim, Woojoo
Kim, Sean M.
Bland, Jeffrey S.
Grayson, Neile
Fang, Mingliang
Meyerhof, Wolfgang
Siuzdak, Gary
Srinivasan, Supriya
Behrens, Maik
Saez, Enrique
author_sort Kok, Bernard P.
collection PubMed
description OBJECTIVES: Extracts of the hops plant have been shown to reduce weight and insulin resistance in rodents and humans, but elucidation of the mechanisms responsible for these benefits has been hindered by the use of heterogeneous hops-derived mixtures. Because hop extracts are used as flavoring agents for their bitter properties, we hypothesized that bitter taste receptors (Tas2rs) could be mediating their beneficial effects in metabolic disease. Studies have shown that exposure of cultured enteroendocrine cells to bitter tastants can stimulate release of hormones, including glucagon-like peptide 1 (GLP-1). These findings have led to the suggestion that activation of Tas2rs may be of benefit in diabetes, but this tenet has not been tested. Here, we have assessed the ability of a pure derivative of a hops isohumulone with anti-diabetic properties, KDT501, to signal through Tas2rs. We have further used this compound as a tool to systematically assess the impact of bitter taste receptor activation in obesity-diabetes. METHODS: KDT501 was tested in a panel of bitter taste receptor signaling assays. Diet-induced obese mice (DIO) were dosed orally with KDT501 and acute effects on glucose homeostasis determined. A wide range of metabolic parameters were evaluated in DIO mice chronically treated with KDT501 to establish the full impact of activating gut bitter taste signaling. RESULTS: We show that KDT501 signals through Tas2r108, one of 35 mouse Tas2rs. In DIO mice, acute treatment stimulated GLP-1 secretion and enhanced glucose tolerance. Chronic treatment caused weight and fat mass loss, increased energy expenditure, enhanced glucose tolerance and insulin sensitivity, normalized plasma lipids, and induced broad suppression of inflammatory markers. Chronic KDT501 treatment altered enteroendocrine hormone levels and bile acid homeostasis and stimulated sustained GLP-1 release. Combined treatment with a dipeptidyl peptidase IV inhibitor amplified the incretin-based benefits of this pure isohumulone. CONCLUSIONS: Activation of Tas2r108 in the gut results in a remodeling of enteroendocrine hormone release and bile acid metabolism that ameliorates multiple features of metabolic syndrome. Targeting extraoral bitter taste receptors may be useful in metabolic disease.
format Online
Article
Text
id pubmed-6158035
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-61580352018-09-27 Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits Kok, Bernard P. Galmozzi, Andrea Littlejohn, Nicole K. Albert, Verena Godio, Cristina Kim, Woojoo Kim, Sean M. Bland, Jeffrey S. Grayson, Neile Fang, Mingliang Meyerhof, Wolfgang Siuzdak, Gary Srinivasan, Supriya Behrens, Maik Saez, Enrique Mol Metab Original Article OBJECTIVES: Extracts of the hops plant have been shown to reduce weight and insulin resistance in rodents and humans, but elucidation of the mechanisms responsible for these benefits has been hindered by the use of heterogeneous hops-derived mixtures. Because hop extracts are used as flavoring agents for their bitter properties, we hypothesized that bitter taste receptors (Tas2rs) could be mediating their beneficial effects in metabolic disease. Studies have shown that exposure of cultured enteroendocrine cells to bitter tastants can stimulate release of hormones, including glucagon-like peptide 1 (GLP-1). These findings have led to the suggestion that activation of Tas2rs may be of benefit in diabetes, but this tenet has not been tested. Here, we have assessed the ability of a pure derivative of a hops isohumulone with anti-diabetic properties, KDT501, to signal through Tas2rs. We have further used this compound as a tool to systematically assess the impact of bitter taste receptor activation in obesity-diabetes. METHODS: KDT501 was tested in a panel of bitter taste receptor signaling assays. Diet-induced obese mice (DIO) were dosed orally with KDT501 and acute effects on glucose homeostasis determined. A wide range of metabolic parameters were evaluated in DIO mice chronically treated with KDT501 to establish the full impact of activating gut bitter taste signaling. RESULTS: We show that KDT501 signals through Tas2r108, one of 35 mouse Tas2rs. In DIO mice, acute treatment stimulated GLP-1 secretion and enhanced glucose tolerance. Chronic treatment caused weight and fat mass loss, increased energy expenditure, enhanced glucose tolerance and insulin sensitivity, normalized plasma lipids, and induced broad suppression of inflammatory markers. Chronic KDT501 treatment altered enteroendocrine hormone levels and bile acid homeostasis and stimulated sustained GLP-1 release. Combined treatment with a dipeptidyl peptidase IV inhibitor amplified the incretin-based benefits of this pure isohumulone. CONCLUSIONS: Activation of Tas2r108 in the gut results in a remodeling of enteroendocrine hormone release and bile acid metabolism that ameliorates multiple features of metabolic syndrome. Targeting extraoral bitter taste receptors may be useful in metabolic disease. Elsevier 2018-08-04 /pmc/articles/PMC6158035/ /pubmed/30120064 http://dx.doi.org/10.1016/j.molmet.2018.07.013 Text en © 2018 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Original Article
Kok, Bernard P.
Galmozzi, Andrea
Littlejohn, Nicole K.
Albert, Verena
Godio, Cristina
Kim, Woojoo
Kim, Sean M.
Bland, Jeffrey S.
Grayson, Neile
Fang, Mingliang
Meyerhof, Wolfgang
Siuzdak, Gary
Srinivasan, Supriya
Behrens, Maik
Saez, Enrique
Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title_full Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title_fullStr Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title_full_unstemmed Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title_short Intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
title_sort intestinal bitter taste receptor activation alters hormone secretion and imparts metabolic benefits
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6158035/
https://www.ncbi.nlm.nih.gov/pubmed/30120064
http://dx.doi.org/10.1016/j.molmet.2018.07.013
work_keys_str_mv AT kokbernardp intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT galmozziandrea intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT littlejohnnicolek intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT albertverena intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT godiocristina intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT kimwoojoo intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT kimseanm intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT blandjeffreys intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT graysonneile intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT fangmingliang intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT meyerhofwolfgang intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT siuzdakgary intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT srinivasansupriya intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT behrensmaik intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits
AT saezenrique intestinalbittertastereceptoractivationaltershormonesecretionandimpartsmetabolicbenefits

Ejemplares similares