A novel DPP IV-resistant C-terminally extended glucagon analogue exhibits weight-lowering and diabetes-protective effects in high-fat-fed mice mediated through glucagon and GLP-1 receptor activation

Lynch, AM; Pathak, Nupur; Pathak, Varun; O’Harte, Finbarr; Flatt, Peter R.; Irwin, Nigel; Gault, Victor

doi:10.1007/s00125-014-3296-7

Cited by 22 publications

(20 citation statements)

References 41 publications

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“…We performed indirect calorimetry studies, illustrating a switch of substrate preference during chronic treatment with dual GLP‐1R/GCGR agonists, starting with preferred fat oxidation and gradually increasing carbohydrate oxidation. The incidence of increased oxygen consumption and energy expenditure during chronic treatment of DIO mice with dual GLP‐1R/GCGR agonists is not novel and has been shown in previous studies . While Day and colleagues observed a tendency toward a decreased respiratory exchange ratio (RER or RQ, respiratory quotient), Lynch et al claimed that RER remained unchanged .…”

Section: Discussionmentioning

confidence: 53%

“…The incidence of increased oxygen consumption and energy expenditure during chronic treatment of DIO mice with dual GLP‐1R/GCGR agonists is not novel and has been shown in previous studies . While Day and colleagues observed a tendency toward a decreased respiratory exchange ratio (RER or RQ, respiratory quotient), Lynch et al claimed that RER remained unchanged . Our results confirmed the latter observations during chronic treatment.…”

Section: Discussionmentioning

confidence: 97%

“…Subsequent clinical studies of oxyntomodulin demonstrated significant efficacy concerning weight loss, resulting from the combined reduction of energy intake and increase of energy expenditure . As natural gastrointestinal hormones such as GLP‐1, glucagon or oxyntomodulin are rapidly degraded by serum proteases and are renally cleared, a number of stabilized oxyntomodulin analogs, as well as GLP‐1R/GCGR dual agonists based on glucagon, have been described as therapeutic agents for the management of obesity and associated metabolic disorders such as type 2 diabetes. However, the apparent challenge associated with translating the beneficial weight loss associated with a dual GLP‐1R/GCGR agonist is to curb the potential glucose‐elevating effects associated with excess glucagon pharmacology.…”

Section: Discussionmentioning

confidence: 99%

“…However, as the elevated fat oxidation should decrease RER further, the increased carbohydrate oxidation apparently compensates for the expected decrease in the case of a dual mouse‐specific agonist. The increased energy expenditure could be linked, only in part, to increased locomotor activity, but others did not report an elevation in spontaneous physical activity . However, our results can provide further clarification by matching the increased energy expenditure to the additional carbohydrate oxidation obtained from GCGR‐stimulated carbohydrate release from hepatic storage.…”

Section: Discussionmentioning

confidence: 99%

“…*P < .01 dual agonist vs vehicle control. #P < .01 dual agonist vs liraglutide (days −7 to 0, days 1 to 3, days 4 to 6, days 7 to 9, days 10 to 45) cleared, a number of stabilized oxyntomodulin analogs,10,28,34 as well as GLP-1R/GCGR dual agonists based on glucagon,8,12,14,[35][36][37] have been described as therapeutic agents for the management of obesity and associated metabolic disorders such as type 2 diabetes. However, the apparent challenge associated with translating the beneficial weight loss associated with a dual GLP-1R/GCGR agonist is to curb the potential glucose-elevating effects associated with excess glucagon pharmacology.…”

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confidence: 99%

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Running on mixed fuel‐dual agonistic approach of GLP‐1 and GCG receptors leads to beneficial impact on body weight and blood glucose control: A comparative study between mice and non‐human primates

Elvert

Herling

Bossart

et al. 2018

Diabetes Obesity Metabolism

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AimWe performed acute and chronic studies in healthy and diet‐induced obese animals using mouse‐specific or monkey‐specific dual GLP‐1R/GCGR agonists to investigate their effects on food intake, body weight, blood glucose control and insulin secretion. The selective GLP‐1R agonist liraglutide was used as comparator.MethodsThe mouse‐specific dual agonist and liraglutide were tested in lean wild type, GLP‐1R knockout and diet‐induced obese mice at different doses. A chronic study was performed in DIO mice to investigate the effect on body weight, food consumption and total energy expenditure (TEE) in obese and diabetic monkeys with a focus on body weight and energy intake.ResultsThe mouse‐specific dual agonist and liraglutide similarly affected glycaemic control. A higher loss in body weight was measured in dual agonist‐treated obese mice. The dual agonist significantly enhanced plasma glucose excursion in overnight fed GLP‐1R−/− mice, probably reflecting a potent GCGR agonist activity. It increased TEE and enhanced fat and carbohydrate oxidation, while liraglutide produced no effect on TEE. In obese and diabetic monkeys, treatment with the monkey‐specific dual agonist reduced total energy intake to 60%‐70% of baseline TEI during chronic treatment. A decrease in body weight and significant improvement in glucose tolerance was observed.ConclusionsIn DIO mice and non‐human primates, dual agonists elicited robust glycaemic control, similar to the marketed GLP‐1R agonist, while eliciting greater effects on body weight. Results from DIO mice suggest that the increase in TEE is caused not only by increased fat oxidation but also by an increase in carbohydrate oxidation.

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Section: Discussionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Running on mixed fuel‐dual agonistic approach of GLP‐1 and GCG receptors leads to beneficial impact on body weight and blood glucose control: A comparative study between mice and non‐human primates

Elvert

Herling

Bossart

et al. 2018

Diabetes Obesity Metabolism

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Population Pharmacokinetics of Cotadutide in Subjects with Type 2 Diabetes

Guan

et al. 2022

Clin Pharmacokinet

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Development and characterisation of a peptidergic N-and C-terminally stabilised mammalian NPY1R agonist which protects against diabetes induction

Lafferty

Tanday

Flatt

et al. 2020

Biochimica et Biophysica Acta (BBA) - General Subjects

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Background: PYY(1-36) peptides from phylogenetically ancient fish, such as sea lamprey, have previously been shown to function as specific neuropeptide Y1 receptor (NPYR1) agonists. Although, sea lamprey PYY(1-36) is N-terminally stable, we reveal in this study that the peptide is subject to endopeptidase mediated C-terminal dipeptide degradation. In an attempt to prevent this, (D-Arg 35)-sea lamprey PYY(1-36) was developed Methods: In vitro bioassays assessed enzymatic stability, insulinostatic activity as well as betastudies examined the impact of twice daily administration of sea lamprey PYY(1-36) or (D-Arg 35)-sea lamprey PYY(1-36) in multiple low dose STZ-induced diabetic mice. Results: (D-Arg 35)-sea lamprey PYY(1-36) was fully resistant to plasma enzymatic degradation. The peptide possessed similar significant NPYR1-mediated insulinostatic, as well as positive beta-cell proliferative and anti-apoptotic biological actions, as the parent peptide. Sea lamprey PYY(1-36) and (D-Arg 35)-sea lamprey PYY(1-36) delayed diabetes progression in STZ mice. Both treatment interventions induced a significant decrease in body weight, food and fluid intake as well as glucose and glucagon concentrations. In addition, glucose tolerance, plasma and pancreatic insulin were partially normalised. (D-Arg 35)-sea lamprey PYY(1-36) was significantly more effective than sea lamprey PYY(1-36) in terms of enhancing glucosestimulate insulin release. Both treatments improved pancreatic islet morphology, linked to augmented proliferation and decreased apoptosis of beta-cells. Conclusion: We present (D-Arg 35)-sea lamprey PYY(1-36) as the first-in-class N-and Cterminally stable PYY(1-36) peptide analogue. General significance: Enzymatically stable, long-acting PYY(1-36) peptides highlight the therapeutic benefits of sustained activation of NPYR1's in diabetes.

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A novel DPP IV-resistant C-terminally extended glucagon analogue exhibits weight-lowering and diabetes-protective effects in high-fat-fed mice mediated through glucagon and GLP-1 receptor activation

Abstract: This study emphasises the potential of (D-Ser(2))glucagon-exe for the treatment of obesity-related diabetes.

Cited by 22 publications

References 41 publications

Running on mixed fuel‐dual agonistic approach of GLP‐1 and GCG receptors leads to beneficial impact on body weight and blood glucose control: A comparative study between mice and non‐human primates

Running on mixed fuel‐dual agonistic approach of GLP‐1 and GCG receptors leads to beneficial impact on body weight and blood glucose control: A comparative study between mice and non‐human primates

Population Pharmacokinetics of Cotadutide in Subjects with Type 2 Diabetes

Development and characterisation of a peptidergic N-and C-terminally stabilised mammalian NPY1R agonist which protects against diabetes induction

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