Pharmacokinetics, safety, tolerability, and efficacy of cotadutide, a GLP ‐1 and glucagon receptor dual agonist, in phase 1/2 trials in overweight or obese participants of Asian descent with or without T2D

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Akiko Sekikawa ◽  
Hyosung Kim ◽  
Robert A Gasser ◽  
Darren Robertson ◽  
...  
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Author(s):  
Philip D. Ambery ◽  
Sebastian Klammt ◽  
Maximillian G. Posch ◽  
Marcella Petrone ◽  
Wenji Pu ◽  
...  

Diabetes ◽  
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Author(s):  
LUKE K. BURKE ◽  
LEE BROWN ◽  
JEAN-MARTIN LAPOINTE ◽  
MICHAL GRZEGORZ SULIKOWSKI ◽  
ARTHUR R. LEWIS ◽  
...  

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CHRISTOPHER D. CHURCH ◽  
SARAH WILL ◽  
ANISH KONKAR ◽  
JAMES TREVASKIS ◽  
...  

Hepatology ◽  
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Vol 65 (3) ◽  
pp. 950-968 ◽  
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Virginia Pardo ◽  
Laura Ruiz ◽  
Luis Castro-Sánchez ◽  
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MICHAEL W. STUMVOLL ◽  
MAXIMILIAN G. POSCH ◽  
TIM HEISE ◽  
LEONA PLUM-MOERSCHEL ◽  
...  

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MICHELLE BEATON ◽  
SILVIA GUIONAUD ◽  
JAMES P. CONWAY ◽  
JOE GRIMSBY ◽  
CHRISTOPHER J. RHODES ◽  
...  

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Vol 391 (10140) ◽  
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Victoria E Parker ◽  
Michael Stumvoll ◽  
Maximilian G Posch ◽  
Tim Heise ◽  
...  

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Vol 215 (3) ◽  
pp. 335-346 ◽  
Author(s):  
Alessandro Pocai

Oxyntomodulin (OXM) is a peptide secreted from the L cells of the gut following nutrient ingestion. OXM is a dual agonist of the glucagon-like peptide-1 receptor (GLP1R) and the glucagon receptor (GCGR) combining the effects of GLP1 and glucagon to act as a potentially more effective treatment for obesity than GLP1R agonists. Injections of OXM in humans cause a significant reduction in weight and appetite, as well as an increase in energy expenditure. Activation of GCGR is classically associated with an elevation in glucose levels, which would be deleterious in patients with T2DM, but the antidiabetic properties of GLP1R agonism would be expected to counteract this effect. Indeed, OXM administration improved glucose tolerance in diet-induced obese mice. Thus, dual agonists of the GCGR and GLP1R represent a new therapeutic approach for diabetes and obesity with the potential for enhanced weight loss and improvement in glycemic control beyond those of GLP1R agonists.


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PEI AN ◽  
HELENA DENG ◽  
LI LI ◽  
LIQI FENG ◽  
...  

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