Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis

OBJECTIVE: The mechanisms behind the efficacy of bariatric surgery (BS) for treating obesity and type 2 diabetes, particularly with respect to the influence of the small bowel, remain poorly understood. In vitro and animal models are suboptimal with respect to their ability to replicate the human in...

Descripción completa

Detalles Bibliográficos
Autores principales: Hasan, Nesrin M., Johnson, Kelli F., Yin, Jianyi, Baetz, Nicholas W., Fayad, Lea, Sherman, Vadim, Blutt, Sarah E., Estes, Mary K., Kumbhari, Vivek, Zachos, Nicholas C., Kovbasnjuk, Olga
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7770968/
https://www.ncbi.nlm.nih.gov/pubmed/33246140
http://dx.doi.org/10.1016/j.molmet.2020.101129
_version_ 1783629623198744576
author Hasan, Nesrin M.
Johnson, Kelli F.
Yin, Jianyi
Baetz, Nicholas W.
Fayad, Lea
Sherman, Vadim
Blutt, Sarah E.
Estes, Mary K.
Kumbhari, Vivek
Zachos, Nicholas C.
Kovbasnjuk, Olga
author_facet Hasan, Nesrin M.
Johnson, Kelli F.
Yin, Jianyi
Baetz, Nicholas W.
Fayad, Lea
Sherman, Vadim
Blutt, Sarah E.
Estes, Mary K.
Kumbhari, Vivek
Zachos, Nicholas C.
Kovbasnjuk, Olga
author_sort Hasan, Nesrin M.
collection PubMed
description OBJECTIVE: The mechanisms behind the efficacy of bariatric surgery (BS) for treating obesity and type 2 diabetes, particularly with respect to the influence of the small bowel, remain poorly understood. In vitro and animal models are suboptimal with respect to their ability to replicate the human intestinal epithelium under conditions induced by obesity. Human enteroids have the potential to accelerate the development of less invasive anti-obesity therapeutics if they can recapitulate the pathophysiology of obesity. Our aim was to determine whether adult stem cell-derived enteroids preserve obesity-characteristic patient-specific abnormalities in carbohydrate absorption and metabolism. METHODS: We established 24 enteroid lines representing 19 lean, overweight, or morbidly obese patients, including post-BS cases. Dietary glucose absorption and gluconeogenesis in enteroids were measured. The expression of carbohydrate transporters and gluconeogenic enzymes was assessed and a pharmacological approach was used to dissect the specific contribution of each transporter or enzyme to carbohydrate absorption and metabolism, respectively. RESULTS: Four phenotypes representing the relationship between patients’ BMI and intestinal dietary sugar absorption were found, suggesting that human enteroids retain obese patient phenotype heterogeneity. Intestinal glucose absorption and gluconeogenesis were significantly elevated in enteroids from a cohort of obese patients. Elevated glucose absorption was associated with increased expression of SGLT1 and GLUT2, whereas elevated gluconeogenesis was related to increased expression of GLUT5, PEPCK1, and G6Pase. CONCLUSIONS: Obesity phenotypes preserved in human enteroids provide a mechanistic link to aberrant dietary carbohydrate absorption and metabolism. Enteroids can be used as a preclinical platform to understand the pathophysiology of obesity, study the heterogeneity of obesity mechanisms, and identify novel therapeutics.
format Online
Article
Text
id pubmed-7770968
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-77709682020-12-30 Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis Hasan, Nesrin M. Johnson, Kelli F. Yin, Jianyi Baetz, Nicholas W. Fayad, Lea Sherman, Vadim Blutt, Sarah E. Estes, Mary K. Kumbhari, Vivek Zachos, Nicholas C. Kovbasnjuk, Olga Mol Metab Original Article OBJECTIVE: The mechanisms behind the efficacy of bariatric surgery (BS) for treating obesity and type 2 diabetes, particularly with respect to the influence of the small bowel, remain poorly understood. In vitro and animal models are suboptimal with respect to their ability to replicate the human intestinal epithelium under conditions induced by obesity. Human enteroids have the potential to accelerate the development of less invasive anti-obesity therapeutics if they can recapitulate the pathophysiology of obesity. Our aim was to determine whether adult stem cell-derived enteroids preserve obesity-characteristic patient-specific abnormalities in carbohydrate absorption and metabolism. METHODS: We established 24 enteroid lines representing 19 lean, overweight, or morbidly obese patients, including post-BS cases. Dietary glucose absorption and gluconeogenesis in enteroids were measured. The expression of carbohydrate transporters and gluconeogenic enzymes was assessed and a pharmacological approach was used to dissect the specific contribution of each transporter or enzyme to carbohydrate absorption and metabolism, respectively. RESULTS: Four phenotypes representing the relationship between patients’ BMI and intestinal dietary sugar absorption were found, suggesting that human enteroids retain obese patient phenotype heterogeneity. Intestinal glucose absorption and gluconeogenesis were significantly elevated in enteroids from a cohort of obese patients. Elevated glucose absorption was associated with increased expression of SGLT1 and GLUT2, whereas elevated gluconeogenesis was related to increased expression of GLUT5, PEPCK1, and G6Pase. CONCLUSIONS: Obesity phenotypes preserved in human enteroids provide a mechanistic link to aberrant dietary carbohydrate absorption and metabolism. Enteroids can be used as a preclinical platform to understand the pathophysiology of obesity, study the heterogeneity of obesity mechanisms, and identify novel therapeutics. Elsevier 2020-11-25 /pmc/articles/PMC7770968/ /pubmed/33246140 http://dx.doi.org/10.1016/j.molmet.2020.101129 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 Original Article
Hasan, Nesrin M.
Johnson, Kelli F.
Yin, Jianyi
Baetz, Nicholas W.
Fayad, Lea
Sherman, Vadim
Blutt, Sarah E.
Estes, Mary K.
Kumbhari, Vivek
Zachos, Nicholas C.
Kovbasnjuk, Olga
Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title_full Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title_fullStr Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title_full_unstemmed Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title_short Intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: Elevated glucose absorption and gluconeogenesis
title_sort intestinal stem cell-derived enteroids from morbidly obese patients preserve obesity-related phenotypes: elevated glucose absorption and gluconeogenesis
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7770968/
https://www.ncbi.nlm.nih.gov/pubmed/33246140
http://dx.doi.org/10.1016/j.molmet.2020.101129
work_keys_str_mv AT hasannesrinm intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT johnsonkellif intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT yinjianyi intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT baetznicholasw intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT fayadlea intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT shermanvadim intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT bluttsarahe intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT estesmaryk intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT kumbharivivek intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT zachosnicholasc intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis
AT kovbasnjukolga intestinalstemcellderivedenteroidsfrommorbidlyobesepatientspreserveobesityrelatedphenotypeselevatedglucoseabsorptionandgluconeogenesis

Ejemplares similares