Glucagon-like peptide 1 in the pathophysiology and pharmacotherapy of clinical obesity

Anandhakrishnan, Ananthi; Korbonits, Márta

doi:10.4239/wjd.v7.i20.572

Cited by 51 publications

(30 citation statements)

References 211 publications

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“…After RYGBP, GLP-1 increases progressively during the first postoperative year, albeit with considerable delay after improvement in glucose homeostasis and weight loss [5], and therefore, the causative effect of GLP-1 on these changes has been challenged. As reported earlier, the plasma levels of GLP-1 in the short term after RYGBP [34], both our groups present a 30-min peak, with GLP-1 levels increasing tenfold compared with baseline. Similar to GLP-1, RYGBP surgery increases fasting [35] as well as postprandial PYY levels postoperatively compared with lean and obese control subjects [36,37].…”

Section: Discussionsupporting

confidence: 87%

Non-responders After Gastric Bypass Surgery for Morbid Obesity: Peptide Hormones and Glucose Homeostasis

et al. 2019

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Introduction About 20% of patients operated with Roux-en-Y gastric bypass (RYGBP) experience poor long-term weight result. This study compared levels of leptin and gut hormones in long-term weight responders with non-responders after RYGBP. In a subgroup analysis, hormone levels were assessed in T2DM (type 2 diabetes mellitus) and normoglycemic participants. Methods Insulin, glucose, leptin, acyl-ghrelin, total PYY, active GLP-1, and GIP were measured during an oral glucose tolerance test (OGTT) in post-RYGBP subjects: 22 non-responders (BMI 40.6 ± 6.0 kg/m 2 after an excess BMI loss [EBMIL] of 26.0 ± 15.9%) and 18 responders (BMI 29.5 ± 3.5 kg/m 2 after an EBMIL of 74.9 ± 18.2%). Subjects were matched for preoperative age, BMI, and years of follow-up. Measures of glucose homeostasis were calculated, and body composition was measured. Results Fat mass-adjusted fasting leptin correlated negatively with %EBMIL (r = − 0.57, p < 0.01). Non-responders presented higher levels of leptin during the OGTT. Leptin decreased and ghrelin returned to baseline levels earlier in non-responders. Despite having higher insulin resistance than responders, non-responders demonstrated similar OGTT responses of GLP-1, GIP, and PYY. T2DM participants demonstrated lower GLP-1 levels than normoglycemic participants of similar weight. Conclusion Fasting leptin is associated with weight result after RYGBP, and hormonal responses to a glucose oral load might work towards promoting obesity in long-term non-responders after RYGBP. Poor long-term weight result and glycemic status after RYGBP are each associated with differences in peptide hormone levels.

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Section: Discussionsupporting

confidence: 87%

Non-responders After Gastric Bypass Surgery for Morbid Obesity: Peptide Hormones and Glucose Homeostasis

et al. 2019

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“…GLP‐1 is a hormone primarily synthesized by the neuroendocrine L‐cells of the ileum and colon and is released in response to food intake . Abnormalities in the postprandial secretion of GLP‐1 have been linked to the pathophysiology of obesity and T2DM . As a potential strategy to enhance GLP‐1 actions, a number of studies have investigated the metabolic effects of GLP‐1 receptor agonists.…”

Section: Resultsmentioning

confidence: 99%

“…As a potential strategy to enhance GLP‐1 actions, a number of studies have investigated the metabolic effects of GLP‐1 receptor agonists. Intravenously administered GLP‐1 receptor agonists (eg, liraglutide and exenatide) have been shown to delay gastric emptying and suppress appetite, which results in clinically meaningful weight loss, with no apparent cardiovascular or psychiatric adverse effects …”

Section: Resultsmentioning

confidence: 99%

Current and emerging therapies for managing hyperphagia and obesity in Prader‐Willi syndrome: A narrative review

et al. 2019

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Summary In early childhood, individuals with Prader‐Willi syndrome (PWS) experience excess weight gain and severe hyperphagia with food compulsivity, which often leads to early onset morbid obesity. Effective treatments for appetite suppression and weight control are currently unavailable for PWS. Our aim to further understand the pathogenesis of PWS led us to carry out a comprehensive search of the current and emerging therapies for managing hyperphagia and extreme weight gain in PWS. A literature search was performed using PubMed and the following keywords: “PWS” AND “therapy” OR “[drug name]”; reference lists, pharmaceutical websites, and the ClinicalTrials.gov registry were also reviewed. Articles presenting data from current standard treatments in PWS and also clinical trials of pharmacological agents in the pipeline were selected. Current standard treatments include dietary restriction/modifications, exercise, and growth hormone replacement, which appear to have limited efficacy for appetite and weight control in patients with PWS. The long‐term safety and effectiveness of bariatric surgery in PWS remains unknown. However, many promising pharmacotherapies are in development and, if approved, will bring much needed choices into the PWS pharmacological armamentarium. With the progress that is currently being made in our understanding of PWS, an effective treatment may not be far off.

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“…Das Polypeptid GLP-1 besteht aus 31 Aminosäuren und wird aus Proglukagon durch das Enzym Prohormonkonvertase 1 abgespalten. Proglukagon wird peripher in den enteroendokrinen L-Zellen und den pankreatischen α-Zellen, sowie zentral in Neuronen des Hirnstamms synthetisiert (2). GLP-1 entsteht dabei überwiegend in den intestinalen L-Zellen (3).…”

Section: Synthese Freisetzung Und Rezeptorbindungunclassified

“…2 min, sodass nur 10-15% des freigesetzten GLP-1 biologisch wirksam die Peripherie erreicht (6). Eine parenterale Gabe von modifiziertem GLP-1 verhindert diesen "first-pass-Effekt" in der Leber (2). Die Wirkung des Hormons wird intrazellulär nach Bindung an einen G-Protein gekoppelten GLP-1-Rezeptor (GLP-1R) vermittelt (7).…”

Section: Synthese Freisetzung Und Rezeptorbindungunclassified

Liraglutid in der Pharmakotherapie der Adipositas

Brede¹,

Lehnert²,

Schmid³

2018

Adipositas - Ursachen, Folgeerkrankungen, Therapie

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ZusammenfassungAufgrund der weltweit zunehmenden Prävalenz von Übergewicht und Adipositas gewinnen medikamentöse Therapien zur Gewichtsreduktion mehr und mehr an Bedeutung. Einen neuen Therapieansatz stellt der Glukagon-like Peptid 1 (GLP-1) Rezeptoragonist Liraglutid dar (Handelsname Saxenda®), der seit März 2015 erstmals zur alleinigen Behandlung der Adipositas in der EU zugelassen ist. Dabei scheinen die gewichtsreduzierenden Effekte von Liraglutid sowohl peripher über eine verzögerte Magenentleerung, als auch zentral über die Beeinflussung von appetitregulierenden Hirnarealen, vermittelt zu sein. In verschiedenen Studien konnte in den letzten Jahren eine signifikante Gewichtsabnahme durch Liraglutid in unterschiedlichen Probandenkollektiven, wie z.B. übergewichtigen und adipösen Patienten ohne aber auch mit Diabetes, nachgewiesen werden. Liraglutid bestätigt sich außerdem als überwiegend gut verträgliche medikamentöse Therapie der Adipositas, wobei die häufigsten berichteten Nebenwirkungen vorübergehende leichte bis moderate gastrointestinale Beschwerden, wie Übelkeit oder Völlegefühl, sind.

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Glucagon-like peptide 1 in the pathophysiology and pharmacotherapy of clinical obesity

Cited by 51 publications

References 211 publications

Non-responders After Gastric Bypass Surgery for Morbid Obesity: Peptide Hormones and Glucose Homeostasis

Non-responders After Gastric Bypass Surgery for Morbid Obesity: Peptide Hormones and Glucose Homeostasis

Current and emerging therapies for managing hyperphagia and obesity in Prader‐Willi syndrome: A narrative review

Liraglutid in der Pharmakotherapie der Adipositas

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