Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps

BACKGROUND: We and others have demonstrated previously that ghrelin receptor (GhrR) knock out (KO) mice fed a high fat diet (HFD) have increased insulin sensitivity and metabolic flexibility relative to WT littermates. A striking feature of the HFD-fed GhrR KO mouse is the dramatic decrease in hepat...

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Autores principales: Qi, Yong, Longo, Kenneth A, Giuliana, Derek J, Gagne, Samantha, McDonagh, Tom, Govek, Elizabeth, Nolan, Anna, Zou, Chaoseng, Morgan, Kristen, Hixon, Jeffrey, Saunders, Jeffrey O, DiStefano, Peter S, Geddes, Brad J
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3024223/
https://www.ncbi.nlm.nih.gov/pubmed/21211044
http://dx.doi.org/10.1186/1472-6793-11-1
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author Qi, Yong
Longo, Kenneth A
Giuliana, Derek J
Gagne, Samantha
McDonagh, Tom
Govek, Elizabeth
Nolan, Anna
Zou, Chaoseng
Morgan, Kristen
Hixon, Jeffrey
Saunders, Jeffrey O
DiStefano, Peter S
Geddes, Brad J
author_facet Qi, Yong
Longo, Kenneth A
Giuliana, Derek J
Gagne, Samantha
McDonagh, Tom
Govek, Elizabeth
Nolan, Anna
Zou, Chaoseng
Morgan, Kristen
Hixon, Jeffrey
Saunders, Jeffrey O
DiStefano, Peter S
Geddes, Brad J
author_sort Qi, Yong
collection PubMed
description BACKGROUND: We and others have demonstrated previously that ghrelin receptor (GhrR) knock out (KO) mice fed a high fat diet (HFD) have increased insulin sensitivity and metabolic flexibility relative to WT littermates. A striking feature of the HFD-fed GhrR KO mouse is the dramatic decrease in hepatic steatosis. To characterize further the underlying mechanisms of glucose homeostasis in GhrR KO mice, we conducted both hyperglycemic (HG) and hyperinsulinemic-euglycemic (HI-E) clamps. Additionally, we investigated tissue glucose uptake and specifically examined liver insulin sensitivity. RESULTS: Consistent with glucose tolerance-test data, in HG clamp experiments, GhrR KO mice showed a reduction in glucose-stimulated insulin release relative to WT littermates. Nevertheless, a robust 1(st )phase insulin secretion was still achieved, indicating that a healthy β-cell response is maintained. Additionally, GhrR KO mice demonstrated both a significantly increased glucose infusion rate and significantly reduced insulin requirement for maintenance of the HG clamp, consistent with their relative insulin sensitivity. In HI-E clamps, both LFD-fed and HFD-fed GhrR KO mice showed higher peripheral insulin sensitivity relative to WT littermates as indicated by a significant increase in insulin-stimulated glucose disposal (Rd), and decreased hepatic glucose production (HGP). HFD-fed GhrR KO mice showed a marked increase in peripheral tissue glucose uptake in a variety of tissues, including skeletal muscle, brown adipose tissue and white adipose tissue. GhrR KO mice fed a HFD also showed a modest, but significant decrease in conversion of pyruvate to glucose, as would be anticipated if these mice displayed increased liver insulin sensitivity. Additionally, the levels of UCP2 and UCP1 were reduced in the liver and BAT, respectively, in GhrR KO mice relative to WT mice. CONCLUSIONS: These results indicate that improved glucose homeostasis of GhrR KO mice is characterized by robust improvements of glucose disposal in both normal and metabolically challenged states, relative to WT controls. GhrR KO mice have an intact 1(st )phase insulin response but require significantly less insulin for glucose disposal. Our experiments reveal that the insulin sensitivity of GhrR KO mice is due to both BW independent and dependent factors. We also provide several lines of evidence that a key feature of the GhrR KO mouse is maintenance of hepatic insulin sensitivity during metabolic challenge.
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spelling pubmed-30242232011-01-21 Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps Qi, Yong Longo, Kenneth A Giuliana, Derek J Gagne, Samantha McDonagh, Tom Govek, Elizabeth Nolan, Anna Zou, Chaoseng Morgan, Kristen Hixon, Jeffrey Saunders, Jeffrey O DiStefano, Peter S Geddes, Brad J BMC Physiol Research Article BACKGROUND: We and others have demonstrated previously that ghrelin receptor (GhrR) knock out (KO) mice fed a high fat diet (HFD) have increased insulin sensitivity and metabolic flexibility relative to WT littermates. A striking feature of the HFD-fed GhrR KO mouse is the dramatic decrease in hepatic steatosis. To characterize further the underlying mechanisms of glucose homeostasis in GhrR KO mice, we conducted both hyperglycemic (HG) and hyperinsulinemic-euglycemic (HI-E) clamps. Additionally, we investigated tissue glucose uptake and specifically examined liver insulin sensitivity. RESULTS: Consistent with glucose tolerance-test data, in HG clamp experiments, GhrR KO mice showed a reduction in glucose-stimulated insulin release relative to WT littermates. Nevertheless, a robust 1(st )phase insulin secretion was still achieved, indicating that a healthy β-cell response is maintained. Additionally, GhrR KO mice demonstrated both a significantly increased glucose infusion rate and significantly reduced insulin requirement for maintenance of the HG clamp, consistent with their relative insulin sensitivity. In HI-E clamps, both LFD-fed and HFD-fed GhrR KO mice showed higher peripheral insulin sensitivity relative to WT littermates as indicated by a significant increase in insulin-stimulated glucose disposal (Rd), and decreased hepatic glucose production (HGP). HFD-fed GhrR KO mice showed a marked increase in peripheral tissue glucose uptake in a variety of tissues, including skeletal muscle, brown adipose tissue and white adipose tissue. GhrR KO mice fed a HFD also showed a modest, but significant decrease in conversion of pyruvate to glucose, as would be anticipated if these mice displayed increased liver insulin sensitivity. Additionally, the levels of UCP2 and UCP1 were reduced in the liver and BAT, respectively, in GhrR KO mice relative to WT mice. CONCLUSIONS: These results indicate that improved glucose homeostasis of GhrR KO mice is characterized by robust improvements of glucose disposal in both normal and metabolically challenged states, relative to WT controls. GhrR KO mice have an intact 1(st )phase insulin response but require significantly less insulin for glucose disposal. Our experiments reveal that the insulin sensitivity of GhrR KO mice is due to both BW independent and dependent factors. We also provide several lines of evidence that a key feature of the GhrR KO mouse is maintenance of hepatic insulin sensitivity during metabolic challenge. BioMed Central 2011-01-06 /pmc/articles/PMC3024223/ /pubmed/21211044 http://dx.doi.org/10.1186/1472-6793-11-1 Text en Copyright ©2011 Qi et al; licensee BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution License (<url>http://creativecommons.org/licenses/by/2.0</url>), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Qi, Yong
Longo, Kenneth A
Giuliana, Derek J
Gagne, Samantha
McDonagh, Tom
Govek, Elizabeth
Nolan, Anna
Zou, Chaoseng
Morgan, Kristen
Hixon, Jeffrey
Saunders, Jeffrey O
DiStefano, Peter S
Geddes, Brad J
Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title_full Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title_fullStr Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title_full_unstemmed Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title_short Characterization of the insulin sensitivity of ghrelin receptor KO mice using glycemic clamps
title_sort characterization of the insulin sensitivity of ghrelin receptor ko mice using glycemic clamps
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3024223/
https://www.ncbi.nlm.nih.gov/pubmed/21211044
http://dx.doi.org/10.1186/1472-6793-11-1
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