GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet

Christoffer Clemmensen; Joseph Chabenne; Brian Finan; Lorraine Sullivan; Katrin Fischer; Daniela Küchler; Laura Sehrer; Teja Ograjsek; Susanna M Hofmann; Sonja C Schriever; Paul T Pfluger; Jason Pinkstaff; Matthias H Tschöp; Richard Dimarchi; Timo D Müller

doi:10.2337/db13-1609

GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet

Christoffer Clemmensen, Joseph Chabenne, Brian Finan, Lorraine Sullivan, Katrin Fischer, Daniela Küchler, Laura Sehrer, Teja Ograjsek, Susanna M Hofmann, Sonja C Schriever, Paul T Pfluger, Jason Pinkstaff, Matthias H Tschöp, Richard Dimarchi, Timo D Müller

90 Citationer (Scopus)

Abstract

We recently reported restoration of leptin responsiveness in diet-induced obese (DIO) mice using a pharmacologically optimized, polyethylene-glycolated (PEG)-leptin analog in combination with exendin-4 or FGF21. However, the return of leptin action required discontinuation of high-fat diet (HFD) exposure. Here we assess whether a single peptide possessing balanced coagonism at the glucagon-like peptide 1 (GLP-1) and glucagon receptors can restore leptin responsiveness in DIO mice maintained on a HFD. DIO mice were treated with PEG-GLP-1/glucagon (30 nmol/kg every fourth day) to induce an ∼15% body weight loss, upon which they were randomized to continue PEG-GLP-1/glucagon therapy or reassigned to receive supplemental daily PEG-leptin (185 nmol/kg/day). The addition of PEG-leptin to PEG-GLP-1/glucagon resulted in an ∼18% greater weight loss as compared with PEG-GLP-1/glucagon alone and was accompanied by further decreases in food intake and improved glucose and lipid metabolism. The beneficial effect of PEG-leptin supplementation occurred after an initial body weight loss similar to what we previously reported following reduced dietary fat along with PEG-leptin and exendin-4 or FGF21 cotreatment. In summary, we report that GLP-1/glucagon coagonism restores leptin responsiveness in mice maintained on a HFD, thus emphasizing the translational value of this polypharmacotherapy for the treatment of obesity and diabetes.

Originalsprog	Engelsk
Tidsskrift	Diabetes
Vol/bind	63
Udgave nummer	4
Sider (fra-til)	1422-7
Antal sider	6
ISSN	0012-1797
DOI	https://doi.org/10.2337/db13-1609
Status	Udgivet - apr. 2014

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10.2337/db13-1609Licens: CC BY-NC-ND

1422.full.pdfForlagets udgivne version, 918 KBLicens: CC BY-NC-ND

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Clemmensen, C., Chabenne, J., Finan, B., Sullivan, L., Fischer, K., Küchler, D., Sehrer, L., Ograjsek, T., Hofmann, S. M., Schriever, S. C., Pfluger, P. T., Pinkstaff, J., Tschöp, M. H., Dimarchi, R., & Müller, T. D. (2014). GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet. Diabetes, 63(4), 1422-7. https://doi.org/10.2337/db13-1609

Clemmensen, C, Chabenne, J, Finan, B, Sullivan, L, Fischer, K, Küchler, D, Sehrer, L, Ograjsek, T, Hofmann, SM, Schriever, SC, Pfluger, PT, Pinkstaff, J, Tschöp, MH, Dimarchi, R & Müller, TD 2014, 'GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet', Diabetes, bind 63, nr. 4, s. 1422-7. https://doi.org/10.2337/db13-1609

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title = "GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet",

abstract = "We recently reported restoration of leptin responsiveness in diet-induced obese (DIO) mice using a pharmacologically optimized, polyethylene-glycolated (PEG)-leptin analog in combination with exendin-4 or FGF21. However, the return of leptin action required discontinuation of high-fat diet (HFD) exposure. Here we assess whether a single peptide possessing balanced coagonism at the glucagon-like peptide 1 (GLP-1) and glucagon receptors can restore leptin responsiveness in DIO mice maintained on a HFD. DIO mice were treated with PEG-GLP-1/glucagon (30 nmol/kg every fourth day) to induce an ∼15% body weight loss, upon which they were randomized to continue PEG-GLP-1/glucagon therapy or reassigned to receive supplemental daily PEG-leptin (185 nmol/kg/day). The addition of PEG-leptin to PEG-GLP-1/glucagon resulted in an ∼18% greater weight loss as compared with PEG-GLP-1/glucagon alone and was accompanied by further decreases in food intake and improved glucose and lipid metabolism. The beneficial effect of PEG-leptin supplementation occurred after an initial body weight loss similar to what we previously reported following reduced dietary fat along with PEG-leptin and exendin-4 or FGF21 cotreatment. In summary, we report that GLP-1/glucagon coagonism restores leptin responsiveness in mice maintained on a HFD, thus emphasizing the translational value of this polypharmacotherapy for the treatment of obesity and diabetes.",

keywords = "Animals, Diet, High-Fat, Eating, Feeding Behavior, Glucagon, Glucagon-Like Peptide 1, Leptin, Male, Mice, Mice, Inbred C57BL, Mice, Obese, Obesity, Polyethylene Glycols, Receptors, Glucagon, Weight Loss, Journal Article, Research Support, Non-U.S. Gov't",

author = "Christoffer Clemmensen and Joseph Chabenne and Brian Finan and Lorraine Sullivan and Katrin Fischer and Daniela K{\"u}chler and Laura Sehrer and Teja Ograjsek and Hofmann, {Susanna M} and Schriever, {Sonja C} and Pfluger, {Paul T} and Jason Pinkstaff and Tsch{\"o}p, {Matthias H} and Richard Dimarchi and M{\"u}ller, {Timo D}",

year = "2014",

month = apr,

doi = "10.2337/db13-1609",

language = "English",

volume = "63",

pages = "1422--7",

journal = "Diabetes",

issn = "0012-1797",

publisher = "American Diabetes Association",

number = "4",

}

TY - JOUR

T1 - GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet

AU - Clemmensen, Christoffer

AU - Chabenne, Joseph

AU - Finan, Brian

AU - Sullivan, Lorraine

AU - Fischer, Katrin

AU - Küchler, Daniela

AU - Sehrer, Laura

AU - Ograjsek, Teja

AU - Hofmann, Susanna M

AU - Schriever, Sonja C

AU - Pfluger, Paul T

AU - Pinkstaff, Jason

AU - Tschöp, Matthias H

AU - Dimarchi, Richard

AU - Müller, Timo D

PY - 2014/4

Y1 - 2014/4

N2 - We recently reported restoration of leptin responsiveness in diet-induced obese (DIO) mice using a pharmacologically optimized, polyethylene-glycolated (PEG)-leptin analog in combination with exendin-4 or FGF21. However, the return of leptin action required discontinuation of high-fat diet (HFD) exposure. Here we assess whether a single peptide possessing balanced coagonism at the glucagon-like peptide 1 (GLP-1) and glucagon receptors can restore leptin responsiveness in DIO mice maintained on a HFD. DIO mice were treated with PEG-GLP-1/glucagon (30 nmol/kg every fourth day) to induce an ∼15% body weight loss, upon which they were randomized to continue PEG-GLP-1/glucagon therapy or reassigned to receive supplemental daily PEG-leptin (185 nmol/kg/day). The addition of PEG-leptin to PEG-GLP-1/glucagon resulted in an ∼18% greater weight loss as compared with PEG-GLP-1/glucagon alone and was accompanied by further decreases in food intake and improved glucose and lipid metabolism. The beneficial effect of PEG-leptin supplementation occurred after an initial body weight loss similar to what we previously reported following reduced dietary fat along with PEG-leptin and exendin-4 or FGF21 cotreatment. In summary, we report that GLP-1/glucagon coagonism restores leptin responsiveness in mice maintained on a HFD, thus emphasizing the translational value of this polypharmacotherapy for the treatment of obesity and diabetes.

AB - We recently reported restoration of leptin responsiveness in diet-induced obese (DIO) mice using a pharmacologically optimized, polyethylene-glycolated (PEG)-leptin analog in combination with exendin-4 or FGF21. However, the return of leptin action required discontinuation of high-fat diet (HFD) exposure. Here we assess whether a single peptide possessing balanced coagonism at the glucagon-like peptide 1 (GLP-1) and glucagon receptors can restore leptin responsiveness in DIO mice maintained on a HFD. DIO mice were treated with PEG-GLP-1/glucagon (30 nmol/kg every fourth day) to induce an ∼15% body weight loss, upon which they were randomized to continue PEG-GLP-1/glucagon therapy or reassigned to receive supplemental daily PEG-leptin (185 nmol/kg/day). The addition of PEG-leptin to PEG-GLP-1/glucagon resulted in an ∼18% greater weight loss as compared with PEG-GLP-1/glucagon alone and was accompanied by further decreases in food intake and improved glucose and lipid metabolism. The beneficial effect of PEG-leptin supplementation occurred after an initial body weight loss similar to what we previously reported following reduced dietary fat along with PEG-leptin and exendin-4 or FGF21 cotreatment. In summary, we report that GLP-1/glucagon coagonism restores leptin responsiveness in mice maintained on a HFD, thus emphasizing the translational value of this polypharmacotherapy for the treatment of obesity and diabetes.

KW - Animals

KW - Diet, High-Fat

KW - Eating

KW - Feeding Behavior

KW - Glucagon

KW - Glucagon-Like Peptide 1

KW - Leptin

KW - Male

KW - Mice

KW - Mice, Inbred C57BL

KW - Mice, Obese

KW - Obesity

KW - Polyethylene Glycols

KW - Receptors, Glucagon

KW - Weight Loss

KW - Journal Article

KW - Research Support, Non-U.S. Gov't

U2 - 10.2337/db13-1609

DO - 10.2337/db13-1609

M3 - Journal article

C2 - 24379349

SN - 0012-1797

VL - 63

SP - 1422

EP - 1427

JO - Diabetes

JF - Diabetes

IS - 4

ER -

GLP-1/glucagon coagonism restores leptin responsiveness in obese mice chronically maintained on an obesogenic diet

Abstract

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