RÉSUMÉ
Dose-scale pharmacodynamic bioequivalence is recommended for evaluating the consistency of generic and innovator formulations of certain locally acting drugs, such as orlistat. This study aimed to investigate the standard methodology for sample size determination and the impact of study design on dose-scale pharmacodynamic bioequivalence using orlistat as the model drug. A population pharmacodynamic model of orlistat was developed using NONMEM 7.5.1 and utilized for subsequent simulations. Three different study designs were evaluated across various predefined relative bioavailability ratios of test/reference (T/R) formulations. These designs included Study Design 1 (2×1 crossover with T1 60 mg, R1 60 mg, and R2 120 mg), Study Design 2 (2×1 crossover with T2 120 mg, R1 60 mg, and R2 120 mg), and Study Design 3 (2×2 crossover with T1 60 mg, T2 120 mg, R1 60 mg, and R2 120 mg). Sample sizes were determined using a stochastic simulation and estimation approach. Under the same T/R ratio and power, Study Design 3 required the minimum sample size for bioequivalence, followed by Study Design 1, while Study Design 2 performed the worst. For Study Designs 1 and 3, a larger sample size was needed on the T/R ratio < 1.0 side for the same power compared to that on the T/R ratio > 1.0 side. The opposite asymmetry was observed for Study Design 2. We demonstrated that Study Design 3 is most effective for reducing the sample size for orlistat bioequivalence studies, and the impact of T/R ratio on sample size shows asymmetry.
Sujet(s)
Études croisées , Orlistat , Équivalence thérapeutique , Orlistat/pharmacocinétique , Orlistat/administration et posologie , Humains , Taille de l'échantillon , Plan de recherche , Biodisponibilité , Modèles biologiques , Agents antiobésité/pharmacocinétique , Agents antiobésité/administration et posologie , Lactones/pharmacocinétique , Lactones/administration et posologie , Simulation numérique , Relation dose-effet des médicamentsRÉSUMÉ
Some thermal degradants of curcuminoids have demonstrated moderate health benefits in previous studies. Feruloyl acetone (FER), recently identified as a thermal degradant of curcumin, has been previously associated with anticancer and antioxidative effects, yet its other capabilities remain unexplored. Moreover, earlier reports suggest that methoxy groups on the aromatic ring may influence the functionality of the curcuminoids. To address these gaps, an animal study was conducted to investigate the antiobesity effects of both FER and its demethoxy counterpart (DFER) on mice subjected to a high-fat diet. The results demonstrated the significant prevention of weight gain and enlargement of the liver and various adipose tissues by both samples. Furthermore, these supplements exhibited a lipid regulatory effect in the liver through the adiponectin/AMPK/SIRT1 pathway, promoted thermogenesis via AMPK/PGC-1α activation, and positively influenced gut-microbial-produced short-chain fatty acid (SCFA) levels. Notably, DFER demonstrated superior overall efficacy in combating obesity, while FER displayed a significant effect in modulating inflammatory responses. It is considered that SCFA may be responsible for the distinct effects of FER and DFER in the animal study. Future studies are anticipated to delve into the efficacy of curcuminoid degradants, encompassing toxicity and pharmacokinetic evaluations.
Sujet(s)
Agents antiobésité , Curcumine , Alimentation riche en graisse , Souris de lignée C57BL , Obésité , Animaux , Curcumine/composition chimique , Curcumine/pharmacologie , Curcumine/métabolisme , Souris , Obésité/métabolisme , Obésité/traitement médicamenteux , Mâle , Agents antiobésité/composition chimique , Agents antiobésité/administration et posologie , Humains , Alimentation riche en graisse/effets indésirables , Foie/métabolisme , Foie/effets des médicaments et des substances chimiques , Foie/composition chimique , Thermogenèse/effets des médicaments et des substances chimiques , Tissu adipeux/effets des médicaments et des substances chimiques , Tissu adipeux/métabolisme , Tissu adipeux/composition chimiqueRÉSUMÉ
OBJECTIVE: The objective of this study was to evaluate the efficacy and safety of semaglutide 2.4 mg, a glucagon-like peptide-1 receptor agonist, by race and ethnicity, across three phase 3 trials. METHODS: The Semaglutide Treatment Effect in People with Obesity (STEP) clinical trials evaluated the efficacy and safety of once-weekly subcutaneous semaglutide 2.4 mg. Here, STEP 1 and 3 data were pooled for analysis; STEP 2 data were examined separately. All analyses were conducted using data from racial and ethnic subgroups. The primary outcome was the estimated treatment difference in percent body weight change for semaglutide 2.4 mg versus placebo. RESULTS: Participants reported race as White (STEP 1 and 3, 75.3%; STEP 2, 59.4%), Black (8.8%; 8.9%), Asian (10.6%; 27.3%), or other racial group (5.3%; 4.4%); and ethnicity as Hispanic or Latino (13.9%; 11.9%) or not Hispanic or Latino (83.9%; 88.1%). There were no significant interactions between treatment effect and race (STEP 1 and 3: p ≥ 0.07; STEP 2: p ≥ 0.15) or ethnicity (p ≥ 0.40; p ≥ 0.85). The safety of semaglutide 2.4 mg was consistent across subgroups. CONCLUSIONS: The treatment effect of semaglutide was statistically significant versus placebo and clinically relevant across all racial and ethnic subgroups in STEP 1 and 3 and STEP 2. All subgroups across both samples demonstrated good tolerability.
Sujet(s)
Peptides glucagon-like , Obésité , Humains , Peptides glucagon-like/administration et posologie , Peptides glucagon-like/effets indésirables , Peptides glucagon-like/usage thérapeutique , Mâle , Femelle , Adulte , Adulte d'âge moyen , Obésité/traitement médicamenteux , Obésité/ethnologie , Résultat thérapeutique , Perte de poids/effets des médicaments et des substances chimiques , Injections sous-cutanées , Méthode en double aveugle , Récepteur du peptide-1 similaire au glucagon/agonistes , , Hispanique ou Latino/statistiques et données numériques , Agents antiobésité/effets indésirables , Agents antiobésité/usage thérapeutique , Agents antiobésité/administration et posologie , Ethnies , Hypoglycémiants/usage thérapeutique , Hypoglycémiants/administration et posologie , Hypoglycémiants/effets indésirablesRÉSUMÉ
This study uses data from US retail pharmacies to assess national GLP-1RA dispensing to adolescents and young adults from 2020-2023.
Sujet(s)
Diabète de type 2 , Ordonnances médicamenteuses , , Obésité , Adolescent , Humains , Jeune adulte , Diabète de type 2/traitement médicamenteux , Récepteur du peptide-1 similaire au glucagon/agonistes , /administration et posologie , /ressources et distribution , /usage thérapeutique , Hypoglycémiants/administration et posologie , Hypoglycémiants/ressources et distribution , Hypoglycémiants/usage thérapeutique , États-Unis/épidémiologie , Food and Drug Administration (USA) , Obésité/traitement médicamenteux , Agents antiobésité/administration et posologie , Agents antiobésité/ressources et distribution , Agents antiobésité/usage thérapeutique , Enfant , Adulte , Ordonnances médicamenteuses/statistiques et données numériques , Mâle , FemelleRÉSUMÉ
OBJECTIVE: Obesity presents an enduring and multifaceted dilemma that impacts individuals, society, economies, and healthcare systems alike. Glucagon-like peptide-1 (GLP-1) receptor agonists, including liraglutide and semaglutide, have received FDA approval for obesity treatment. This study aims to present a cost-effectiveness analysis to compare the cost and clinical outcomes of semaglutide vs. liraglutide on weight loss in people with overweight and obesity. MATERIALS AND METHODS: A cost-effectiveness analysis was conducted to compare the cost and the clinical outcomes of adding weekly 2.4 mg SC semaglutide vs. daily 3.0 mg SC liraglutide or placebo to physical activity and diet control in overweight and obese patients. A clinical outcome of achieving ≥15% weight loss was chosen. A simple decision analysis model from a third-payer perspective was applied. Drug costs were based on the retail price of the USA market. One-way sensitivity analyses were performed. RESULTS: Results showed that 2.4 mg weekly semaglutide, when added to physical activity and diet control, was the most cost-effective choice in terms of ≥15% weight loss (ICER: $ 7,056/patient/68 weeks). The model was robust against the 50% increase in the unit cost of semaglutide and the 50% decrease in the unit cost of liraglutide, as well as the changes in probabilities by the corresponding 95% confidence intervals across the model. CONCLUSIONS: This cost-effectiveness analysis suggests that employing once-weekly 2.4 mg semaglutide emerges as a remarkably cost-effective option when contrasted with once-daily 3.0 mg liraglutide in patients with overweight and obesity when added to physical activity and diet control.
Sujet(s)
Analyse coût-bénéfice , Peptides glucagon-like , Liraglutide , Obésité , Surpoids , Humains , Peptides glucagon-like/économie , Peptides glucagon-like/administration et posologie , Peptides glucagon-like/usage thérapeutique , Liraglutide/administration et posologie , Liraglutide/économie , Liraglutide/usage thérapeutique , Obésité/traitement médicamenteux , Obésité/économie , Surpoids/traitement médicamenteux , Surpoids/économie , Injections sous-cutanées , Techniques d'aide à la décision , Perte de poids/effets des médicaments et des substances chimiques , Calendrier d'administration des médicaments , Agents antiobésité/économie , Agents antiobésité/administration et posologie , Agents antiobésité/usage thérapeutique , Hypoglycémiants/économie , Hypoglycémiants/administration et posologie , Hypoglycémiants/usage thérapeutique , Évaluation du Coût-EfficacitéRÉSUMÉ
This JAMA Internal Medicine Patient Page describes how to use injectable weight-loss medications as well as their risks and benefits.
Sujet(s)
Agents antiobésité , Humains , Agents antiobésité/usage thérapeutique , Agents antiobésité/administration et posologie , Obésité , Perte de poids/effets des médicaments et des substances chimiques , InjectionsRÉSUMÉ
Obesity is a threat to public health and effective new medications are required. Platycodonis Radix (PR) is a traditional medicinal/dietary plant with activities against obesity. Using mice given a diet rich in fat, the antiobesity components of PR were identified and their molecular mechanisms were clarified further in this investigation. Initially, the impacts of PR fractions on liver histology and biochemical markers were assessed. Subsequently, the degrees of lipogenic and lipolytic gene and protein expressions were determined. Oral administration of PR polysaccharides (PG) (0.80 g/kg body weight) improved liver function (alanine aminotransferase and aspartate aminotransferase) and its antioxidant activities (total superoxide dismutase, glutathione peroxidase, and malondialdehyde), as well as alleviated blood lipid (total cholesterol, total triglyceride, high-density lipoprotein cholesterol, and low-density lipoprotein cholesterol) values, inflammatory systemic (TNF-α and IL-1ß), and histological abnormalities within the liver. Furthermore, PG administration downregulated the expression for lipogenic genes (ACC and FAS) and upregulated the expression for the lipolytic gene (PPARα, LPL, CPT1, and HSL). Importantly, PG raised AMPK phosphorylation and decreased SREBP-1c protein synthesis. Thus, it is possible that PG stimulates the AMPK-LPL/HSL path (lipolytic route) plus the AMPK-ACC/PPARα-CPT1 path (associated to ß-oxidation of fatty acids), while inhibiting the AMPK/(SREBP-1c)-ACC/FAS path (lipogenic route). In summary, PG has the ability to regulate lipid metabolism, and it may be useful to pharmacologically activate AMPK with PG to prevent and cure obesity.
Sujet(s)
Agents antiobésité , Alimentation riche en graisse , Foie , Souris de lignée C57BL , Obésité , Extraits de plantes , Platycodon , Animaux , Alimentation riche en graisse/effets indésirables , Obésité/métabolisme , Obésité/traitement médicamenteux , Mâle , Agents antiobésité/pharmacologie , Agents antiobésité/administration et posologie , Souris , Platycodon/composition chimique , Foie/effets des médicaments et des substances chimiques , Foie/métabolisme , Extraits de plantes/pharmacologie , Extraits de plantes/administration et posologie , Humains , Protéine-1 de liaison à l'élément de régulation des stérols/métabolisme , Protéine-1 de liaison à l'élément de régulation des stérols/génétique , Racines de plante/composition chimique , Récepteur PPAR alpha/métabolisme , Récepteur PPAR alpha/génétique , Facteur de nécrose tumorale alpha/métabolisme , Facteur de nécrose tumorale alpha/génétique , Polyosides/pharmacologie , Polyosides/administration et posologie , Lipogenèse/effets des médicaments et des substances chimiques , Lipolyse/effets des médicaments et des substances chimiques , Triglycéride/métabolisme , Triglycéride/sang , Alanine transaminase/métabolisme , Alanine transaminase/sangRÉSUMÉ
BACKGROUND: Dietary intervention, including polyphenol consumption, is recognized as an effective strategy to prevent obesity. Although fermented jujube juice (FJJ) with lactic acid bacteria has been shown to be rich in polyphenols and have strong antioxidant properties, little is known about its anti-obesity properties. RESULTS: Untargeted metabolomics was employed to identify and analyze the differential metabolites between FJJ and raw jujube juice. A total of 431 metabolites belonging to diverse classes and with various functional active ingredients were quantitatively identified. The animal experiments results showed that FJJ administration for 13 weeks significantly inhibited high-fat-diet-induced body and epididymal adipose weight gain, and improved the serum lipid parameters in obese mice. Additionally, DNA-sequencing results revealed that FJJ treatment increased Akkermansia abundance in the gut and changed the composition of fecal microbiota by decreasing the Firmicutes/Bacteroidota ratio and Helicobacter pylori abundance. CONCLUSION: These findings suggest that FJJ contributes to regulating lipid accumulation and gut microbiota composition in high-fat-diet-induced obese mice, which helps to prevent obesity. Hence, FJJ has the potential to be a beneficial beverage for controlling obesity. © 2024 Society of Chemical Industry.
Sujet(s)
Agents antiobésité , Alimentation riche en graisse , Jus de fruits et de légumes , Microbiome gastro-intestinal , Métabolomique , Souris de lignée C57BL , Souris obèse , Obésité , Probiotiques , Ziziphus , Animaux , Alimentation riche en graisse/effets indésirables , Obésité/métabolisme , Obésité/diétothérapie , Obésité/microbiologie , Souris , Jus de fruits et de légumes/analyse , Mâle , Microbiome gastro-intestinal/effets des médicaments et des substances chimiques , Ziziphus/composition chimique , Probiotiques/administration et posologie , Probiotiques/pharmacologie , Agents antiobésité/administration et posologie , Agents antiobésité/pharmacologie , Bactéries/classification , Bactéries/isolement et purification , Bactéries/génétique , Bactéries/métabolisme , HumainsRÉSUMÉ
BACKGROUND: Yellow leaf green tea (YLGT) is a new variety of Camellia sinensis (L.) O. Ktze, which has yellow leaves and the unique qualities of 'three green through three yellow'. The present study aimed to investigate the anti-obesity effect of YLGT in mice fed a high-fat diet (HFD) and to explore the potential mechanisms by regulating the AMPK/ACC/SREBP1c signaling pathways and gut microbiota. RESULTS: The results showed that YLGT aqueous extract reduced body weight, hepatic inflammation, fat accumulation and hyperlipidemia in HFD-induced C57BL/6J mice, and also accelerated energy metabolism, reduced fat synthesis and suppressed obesity by activating the AMPK/CPT-1α signaling pathway and inhibiting the FAS/ACC/SREBP-1c signaling pathway. Fecal microbiota transplantation experiment further confirmed that the alteration of gut microbiota (e.g. increasing unclassified_Muribaculaceae and decreasing Colidextribacter) might be an important cause of YLGT water extract inhibiting obesity. CONCLUSION: In conclusion, YLGT has a broad application prospect in the treatment of obesity and the development of anti-obesity function beverages. © 2024 Society of Chemical Industry.
Sujet(s)
AMP-Activated Protein Kinases , Camellia sinensis , Alimentation riche en graisse , Microbiome gastro-intestinal , Souris de lignée C57BL , Obésité , Extraits de plantes , Feuilles de plante , Transduction du signal , Protéine-1 de liaison à l'élément de régulation des stérols , Animaux , Microbiome gastro-intestinal/effets des médicaments et des substances chimiques , Alimentation riche en graisse/effets indésirables , Obésité/métabolisme , Obésité/microbiologie , Obésité/traitement médicamenteux , Obésité/diétothérapie , Souris , Camellia sinensis/composition chimique , Mâle , Transduction du signal/effets des médicaments et des substances chimiques , Feuilles de plante/composition chimique , Extraits de plantes/pharmacologie , Extraits de plantes/composition chimique , AMP-Activated Protein Kinases/métabolisme , Protéine-1 de liaison à l'élément de régulation des stérols/métabolisme , Protéine-1 de liaison à l'élément de régulation des stérols/génétique , Humains , Acetyl-coA carboxylase/métabolisme , Acetyl-coA carboxylase/génétique , Thé/composition chimique , Bactéries/classification , Bactéries/génétique , Bactéries/isolement et purification , Bactéries/effets des médicaments et des substances chimiques , Bactéries/métabolisme , Foie/métabolisme , Foie/effets des médicaments et des substances chimiques , Agents antiobésité/pharmacologie , Agents antiobésité/administration et posologieSujet(s)
Peptides glucagon-like , Perte de poids , Peptides glucagon-like/administration et posologie , Peptides glucagon-like/effets indésirables , Peptides glucagon-like/usage thérapeutique , Humains , Perte de poids/effets des médicaments et des substances chimiques , Administration par voie orale , Obésité/traitement médicamenteux , Résultat thérapeutique , Agents antiobésité/administration et posologie , Agents antiobésité/effets indésirablesRÉSUMÉ
Importance: The effect of continued treatment with tirzepatide on maintaining initial weight reduction is unknown. Objective: To assess the effect of tirzepatide, with diet and physical activity, on the maintenance of weight reduction. Design, Setting, and Participants: This phase 3, randomized withdrawal clinical trial conducted at 70 sites in 4 countries with a 36-week, open-label tirzepatide lead-in period followed by a 52-week, double-blind, placebo-controlled period included adults with a body mass index greater than or equal to 30 or greater than or equal to 27 and a weight-related complication, excluding diabetes. Interventions: Participants (n = 783) enrolled in an open-label lead-in period received once-weekly subcutaneous maximum tolerated dose (10 or 15 mg) of tirzepatide for 36 weeks. At week 36, a total of 670 participants were randomized (1:1) to continue receiving tirzepatide (n = 335) or switch to placebo (n = 335) for 52 weeks. Main Outcomes and Measures: The primary end point was the mean percent change in weight from week 36 (randomization) to week 88. Key secondary end points included the proportion of participants at week 88 who maintained at least 80% of the weight loss during the lead-in period. Results: Participants (n = 670; mean age, 48 years; 473 [71%] women; mean weight, 107.3 kg) who completed the 36-week lead-in period experienced a mean weight reduction of 20.9%. The mean percent weight change from week 36 to week 88 was -5.5% with tirzepatide vs 14.0% with placebo (difference, -19.4% [95% CI, -21.2% to -17.7%]; P < .001). Overall, 300 participants (89.5%) receiving tirzepatide at 88 weeks maintained at least 80% of the weight loss during the lead-in period compared with 16.6% receiving placebo (P < .001). The overall mean weight reduction from week 0 to 88 was 25.3% for tirzepatide and 9.9% for placebo. The most common adverse events were mostly mild to moderate gastrointestinal events, which occurred more commonly with tirzepatide vs placebo. Conclusions and Relevance: In participants with obesity or overweight, withdrawing tirzepatide led to substantial regain of lost weight, whereas continued treatment maintained and augmented initial weight reduction. Trial Registration: ClinicalTrials.gov Identifier: NCT04660643.
Sujet(s)
Agents antiobésité , Obésité , Perte de poids , Adulte , Femelle , Humains , Mâle , Adulte d'âge moyen , Méthode en double aveugle , Peptide gastrointestinal/administration et posologie , Peptide gastrointestinal/effets indésirables , Peptide gastrointestinal/pharmacologie , Peptide gastrointestinal/usage thérapeutique , Obésité/traitement médicamenteux , Obésité/complications , Surpoids/complications , Surpoids/traitement médicamenteux , Résultat thérapeutique , Perte de poids/effets des médicaments et des substances chimiques , Récepteur du peptide-2 similaire au glucagon/administration et posologie , Récepteur du peptide-2 similaire au glucagon/agonistes , Récepteur du peptide-2 similaire au glucagon/usage thérapeutique , Incrétines/administration et posologie , Incrétines/effets indésirables , Incrétines/pharmacologie , Incrétines/usage thérapeutique , Agents antiobésité/administration et posologie , Agents antiobésité/effets indésirables , Agents antiobésité/pharmacologie , Agents antiobésité/usage thérapeutique , Chimiothérapie de maintenance , Injections sous-cutanées , Abstention thérapeutiqueRÉSUMÉ
BACKGROUND: Obesity is a major risk factor for many leading causes of illness and death worldwide. Data are needed regarding the efficacy and safety of the nonpeptide glucagon-like peptide-1 (GLP-1) receptor agonist orforglipron as a once-daily oral therapy for weight reduction in adults with obesity. METHODS: In this phase 2, randomized, double-blind trial, we enrolled adults with obesity, or with overweight plus at least one weight-related coexisting condition, and without diabetes. Participants were randomly assigned to receive orforglipron at one of four doses (12, 24, 36, or 45 mg) or placebo once daily for 36 weeks. The percentage change from baseline in body weight was assessed at week 26 (primary end point) and at week 36 (secondary end point). RESULTS: A total of 272 participants underwent randomization. At baseline, the mean body weight was 108.7 kg, and the mean body-mass index (the weight in kilograms divided by the square of the height in meters) was 37.9. At week 26, the mean change from baseline in body weight ranged from -8.6% to -12.6% across the orforglipron dose cohorts and was -2.0% in the placebo group. At week 36, the mean change ranged from -9.4% to -14.7% with orforglipron and was -2.3% with placebo. A weight reduction of at least 10% by week 36 occurred in 46 to 75% of the participants who received orforglipron, as compared with 9% who received placebo. The use of orforglipron led to improvement in all prespecified weight-related and cardiometabolic measures. The most common adverse events reported with orforglipron were gastrointestinal events, which were mild to moderate, occurred primarily during dose escalation, and led to discontinuation of orforglipron in 10 to 17% of participants across dose cohorts. The safety profile of orforglipron was consistent with that of the GLP-1 receptor agonist class. CONCLUSIONS: Daily oral orforglipron, a nonpeptide GLP-1 receptor agonist, was associated with weight reduction. Adverse events reported with orforglipron were similar to those with injectable GLP-1 receptor agonists. (Funded by Eli Lilly; GZGI ClinicalTrials.gov number, NCT05051579.).
Sujet(s)
Agents antiobésité , Récepteur du peptide-1 similaire au glucagon , Obésité , Perte de poids , Adulte , Humains , Administration par voie orale , Agents antiobésité/administration et posologie , Agents antiobésité/effets indésirables , Agents antiobésité/pharmacologie , Agents antiobésité/usage thérapeutique , Diabète de type 2 , Méthode en double aveugle , Récepteur du peptide-1 similaire au glucagon/agonistes , Peptides glucagon-like , Hypoglycémiants/usage thérapeutique , Obésité/complications , Obésité/traitement médicamenteux , Obésité/induit chimiquement , Perte de poids/effets des médicaments et des substances chimiquesRÉSUMÉ
BACKGROUND: Retatrutide (LY3437943) is an agonist of the glucose-dependent insulinotropic polypeptide, glucagon-like peptide 1, and glucagon receptors. Its dose-response relationships with respect to side effects, safety, and efficacy for the treatment of obesity are not known. METHODS: We conducted a phase 2, double-blind, randomized, placebo-controlled trial involving adults who had a body-mass index (BMI, the weight in kilograms divided by the square of the height in meters) of 30 or higher or who had a BMI of 27 to less than 30 plus at least one weight-related condition. Participants were randomly assigned in a 2:1:1:1:1:2:2 ratio to receive subcutaneous retatrutide (1 mg, 4 mg [initial dose, 2 mg], 4 mg [initial dose, 4 mg], 8 mg [initial dose, 2 mg], 8 mg [initial dose, 4 mg], or 12 mg [initial dose, 2 mg]) or placebo once weekly for 48 weeks. The primary end point was the percentage change in body weight from baseline to 24 weeks. Secondary end points included the percentage change in body weight from baseline to 48 weeks and a weight reduction of 5% or more, 10% or more, or 15% or more. Safety was also assessed. RESULTS: We enrolled 338 adults, 51.8% of whom were men. The least-squares mean percentage change in body weight at 24 weeks in the retatrutide groups was -7.2% in the 1-mg group, -12.9% in the combined 4-mg group, -17.3% in the combined 8-mg group, and -17.5% in the 12-mg group, as compared with -1.6% in the placebo group. At 48 weeks, the least-squares mean percentage change in the retatrutide groups was -8.7% in the 1-mg group, -17.1% in the combined 4-mg group, -22.8% in the combined 8-mg group, and -24.2% in the 12-mg group, as compared with -2.1% in the placebo group. At 48 weeks, a weight reduction of 5% or more, 10% or more, and 15% or more had occurred in 92%, 75%, and 60%, respectively, of the participants who received 4 mg of retatrutide; 100%, 91%, and 75% of those who received 8 mg; 100%, 93%, and 83% of those who received 12 mg; and 27%, 9%, and 2% of those who received placebo. The most common adverse events in the retatrutide groups were gastrointestinal; these events were dose-related, were mostly mild to moderate in severity, and were partially mitigated with a lower starting dose (2 mg vs. 4 mg). Dose-dependent increases in heart rate peaked at 24 weeks and declined thereafter. CONCLUSIONS: In adults with obesity, retatrutide treatment for 48 weeks resulted in substantial reductions in body weight. (Funded by Eli Lilly; ClinicalTrials.gov number, NCT04881760.).
Sujet(s)
Agents antiobésité , Peptide gastrointestinal , Glucagon-like peptide 1 , Obésité , Récepteurs au glucagon , Adulte , Femelle , Humains , Mâle , Indice de masse corporelle , Méthode en double aveugle , Glucagon-like peptide 1/agonistes , Obésité/complications , Obésité/traitement médicamenteux , Résultat thérapeutique , Perte de poids/effets des médicaments et des substances chimiques , Peptide gastrointestinal/agonistes , Récepteurs au glucagon/agonistes , Injections sous-cutanées , Agents antiobésité/administration et posologie , Agents antiobésité/effets indésirables , Agents antiobésité/pharmacologie , Agents antiobésité/usage thérapeutiqueRÉSUMÉ
BACKGROUND: A once-weekly, 2.4-mg dose of subcutaneous semaglutide, a glucagon-like peptide-1 receptor agonist, is used to treat obesity in adults, but assessment of the drug in adolescents has been lacking. METHODS: In this double-blind, parallel-group, randomized, placebo-controlled trial, we enrolled adolescents (12 to <18 years of age) with obesity (a body-mass index [BMI] in the 95th percentile or higher) or with overweight (a BMI in the 85th percentile or higher) and at least one weight-related coexisting condition. Participants were randomly assigned in a 2:1 ratio to receive once-weekly subcutaneous semaglutide (at a dose of 2.4 mg) or placebo for 68 weeks, plus lifestyle intervention. The primary end point was the percentage change in BMI from baseline to week 68; the secondary confirmatory end point was weight loss of at least 5% at week 68. RESULTS: A total of 201 participants underwent randomization, and 180 (90%) completed treatment. All but one of the participants had obesity. The mean change in BMI from baseline to week 68 was -16.1% with semaglutide and 0.6% with placebo (estimated difference, -16.7 percentage points; 95% confidence interval [CI], -20.3 to -13.2; P<0.001). At week 68, a total of 95 of 131 participants (73%) in the semaglutide group had weight loss of 5% or more, as compared with 11 of 62 participants (18%) in the placebo group (estimated odds ratio, 14.0; 95% CI, 6.3 to 31.0; P<0.001). Reductions in body weight and improvement with respect to cardiometabolic risk factors (waist circumference and levels of glycated hemoglobin, lipids [except high-density lipoprotein cholesterol], and alanine aminotransferase) were greater with semaglutide than with placebo. The incidence of gastrointestinal adverse events was greater with semaglutide than with placebo (62% vs. 42%). Five participants (4%) in the semaglutide group and no participants in the placebo group had cholelithiasis. Serious adverse events were reported in 15 of 133 participants (11%) in the semaglutide group and in 6 of 67 participants (9%) in the placebo group. CONCLUSIONS: Among adolescents with obesity, once-weekly treatment with a 2.4-mg dose of semaglutide plus lifestyle intervention resulted in a greater reduction in BMI than lifestyle intervention alone. (Funded by Novo Nordisk; STEP TEENS ClinicalTrials.gov number, NCT04102189.).
Sujet(s)
Agents antiobésité , Obésité pédiatrique , Adolescent , Humains , Méthode en double aveugle , Obésité pédiatrique/traitement médicamenteux , Obésité pédiatrique/thérapie , Perte de poids/effets des médicaments et des substances chimiques , Mode de vie sain , Récepteur du peptide-1 similaire au glucagon/agonistes , Indice de masse corporelle , Agents antiobésité/administration et posologie , Agents antiobésité/effets indésirables , Administration par voie cutanée , EnfantRÉSUMÉ
BACKGROUND: Obesity is a chronic disease that results in substantial global morbidity and mortality. The efficacy and safety of tirzepatide, a novel glucose-dependent insulinotropic polypeptide and glucagon-like peptide-1 receptor agonist, in people with obesity are not known. METHODS: In this phase 3 double-blind, randomized, controlled trial, we assigned 2539 adults with a body-mass index (BMI; the weight in kilograms divided by the square of the height in meters) of 30 or more, or 27 or more and at least one weight-related complication, excluding diabetes, in a 1:1:1:1 ratio to receive once-weekly, subcutaneous tirzepatide (5 mg, 10 mg, or 15 mg) or placebo for 72 weeks, including a 20-week dose-escalation period. Coprimary end points were the percentage change in weight from baseline and a weight reduction of 5% or more. The treatment-regimen estimand assessed effects regardless of treatment discontinuation in the intention-to-treat population. RESULTS: At baseline, the mean body weight was 104.8 kg, the mean BMI was 38.0, and 94.5% of participants had a BMI of 30 or higher. The mean percentage change in weight at week 72 was -15.0% (95% confidence interval [CI], -15.9 to -14.2) with 5-mg weekly doses of tirzepatide, -19.5% (95% CI, -20.4 to -18.5) with 10-mg doses, and -20.9% (95% CI, -21.8 to -19.9) with 15-mg doses and -3.1% (95% CI, -4.3 to -1.9) with placebo (P<0.001 for all comparisons with placebo). The percentage of participants who had weight reduction of 5% or more was 85% (95% CI, 82 to 89), 89% (95% CI, 86 to 92), and 91% (95% CI, 88 to 94) with 5 mg, 10 mg, and 15 mg of tirzepatide, respectively, and 35% (95% CI, 30 to 39) with placebo; 50% (95% CI, 46 to 54) and 57% (95% CI, 53 to 61) of participants in the 10-mg and 15-mg groups had a reduction in body weight of 20% or more, as compared with 3% (95% CI, 1 to 5) in the placebo group (P<0.001 for all comparisons with placebo). Improvements in all prespecified cardiometabolic measures were observed with tirzepatide. The most common adverse events with tirzepatide were gastrointestinal, and most were mild to moderate in severity, occurring primarily during dose escalation. Adverse events caused treatment discontinuation in 4.3%, 7.1%, 6.2%, and 2.6% of participants receiving 5-mg, 10-mg, and 15-mg tirzepatide doses and placebo, respectively. CONCLUSIONS: In this 72-week trial in participants with obesity, 5 mg, 10 mg, or 15 mg of tirzepatide once weekly provided substantial and sustained reductions in body weight. (Supported by Eli Lilly; SURMOUNT-1 ClinicalTrials.gov number, NCT04184622.).
Sujet(s)
Agents antiobésité , Obésité , Perte de poids , Adulte , Agents antiobésité/administration et posologie , Agents antiobésité/pharmacologie , Agents antiobésité/usage thérapeutique , Relation dose-effet des médicaments , Méthode en double aveugle , Peptide gastrointestinal/administration et posologie , Peptide gastrointestinal/usage thérapeutique , Peptides glucagon-like/administration et posologie , Peptides glucagon-like/agonistes , Peptides glucagon-like/usage thérapeutique , Humains , Injections sous-cutanées , Obésité/complications , Obésité/traitement médicamenteux , Résultat thérapeutique , Perte de poids/effets des médicaments et des substances chimiquesRÉSUMÉ
Prolactin-releasing peptide (PrRP) is an endogenous neuropeptide involved in appetite regulation and energy homeostasis. PrRP binds with high affinity to G-protein coupled receptor 10 (GPR10) and with lesser activity towards the neuropeptide FF receptor type 2 (NPFF2R). The present study aimed to develop long-acting PrRP31 analogues with potent anti-obesity efficacy. A comprehensive series of C18 lipidated PrRP31 analogues was characterized in vitro and analogues with various GPR10 and NPFF2R activity profiles were profiled for bioavailability and metabolic effects following subcutaneous administration in diet-induced obese (DIO) mice. PrRP31 analogues acylated with a C18 lipid chain carrying a terminal acid (C18 diacid) were potent GPR10-selective agonists and weight-neutral in DIO mice. In contrast, acylation with aliphatic C18 lipid chain (C18) resulted in dual GPR10-NPFF2R co-agonists that suppressed food intake and promoted a robust weight loss in DIO mice, which was sustained for at least one week after last dosing. Rapid in vivo degradation of C18 PrRP31 analogues gave rise to circulating lipidated PrRP metabolites maintaining dual GPR10-NPFF2R agonist profile and long-acting anti-obesity efficacy in DIO mice. Combined GPR10 and NPFF2R activation may therefore be a critical mechanism for obtaining robust anti-obesity efficacy of PrRP31 analogues.
Sujet(s)
Agents antiobésité/administration et posologie , Obésité/traitement médicamenteux , Hormone de libération de la prolactine/analogues et dérivés , Hormone de libération de la prolactine/administration et posologie , Récepteurs couplés aux protéines G/agonistes , Récepteur aux neuropeptides/agonistes , Perte de poids/effets des médicaments et des substances chimiques , Acylation , Animaux , Régulation de l'appétit/effets des médicaments et des substances chimiques , Alimentation riche en graisse/effets indésirables , Modèles animaux de maladie humaine , Consommation alimentaire/effets des médicaments et des substances chimiques , Mâle , Souris , Souris de lignée C57BL , Obésité/étiologie , Obésité/métabolisme , Hormone de libération de la prolactine/métabolisme , Récepteurs couplés aux protéines G/métabolisme , Récepteur aux neuropeptides/métabolisme , Résultat thérapeutiqueRÉSUMÉ
Obesity has been reported to be associated with gut microbiome dysbiosis. seabuckthorn fruits have traditionally been used in Tibetan foods and medicines for thousands of years. Seabuckthorn polysaccharide (SP) is one of the main functional components in seabuckthorn fruits. However, the effects of SP on a high-fat diet (HFD)-induced obesity have not yet been elucidated. The purpose of this study is to explore the amelioration effect of SP on obesity induced by HFD and to reveal its mechanism of gut microbiota and its metabolites. Results showed that 12-week SP (0.1%, w/w) dietary supplementation could significantly reduce body weight gain, serum lipid level and liver triglycerides level in obese mice. Notably, the SP treatment elevated p-AMPKα and PPARα proteins expression stimulated the phosphorylation of ACC1 and inhibited the protein expression of FAS, PPARγ, and CD36 in the mice liver. Further, SP also reorganized the gut microbiome by up-regulating the proportion of Muribaculaceae_unclassified, Bifidobacterium, Rikenellaceae_RC9_gut_group, Alistipes, and Bacteroides, and down-regulating the abundance of Lactobacillus, Firmicutes_unclassified, Dubosiella Bilophila, and Streptococcus in HFD-induced obese mice. Moreover, the production of microbial metabolites short-chain fatty acids (SCFAs) in feces has also increased. In addition, correlation analysis results showed that obesity-ameliorating effects of SP were highly associated with levels of SCFAs in feces. Therefore, the regulation of SP on liver lipid metabolism may be due to the variation of the gut microbiome and raised production of SCFAs. These results indicate that SP could play the part of a potential nutraceutical for ameliorating obesity through regulation of the gut-liver axis.
Sujet(s)
Agents antiobésité/pharmacologie , Compléments alimentaires , Hippophae , Polyosides/pharmacologie , Animaux , Agents antiobésité/administration et posologie , Agents antiobésité/composition chimique , Alimentation riche en graisse , Modèles animaux de maladie humaine , Microbiome gastro-intestinal/effets des médicaments et des substances chimiques , Métabolisme lipidique/effets des médicaments et des substances chimiques , Foie/métabolisme , Mâle , Souris , Souris de lignée C57BL , Obésité/prévention et contrôle , Polyosides/administration et posologie , Polyosides/composition chimique , Prise de poids/effets des médicaments et des substances chimiquesRÉSUMÉ
BACKGROUND: Pharmacotherapy provides an option for adults with overweight and obesity to reduce their bodyweight if lifestyle modifications fail. We summarised the latest evidence for the benefits and harms of weight-lowering drugs. METHODS: This systematic review and network meta-analysis included searches of PubMed, Embase, and Cochrane Library (CENTRAL) from inception to March 23, 2021, for randomised controlled trials of weight-lowering drugs in adults with overweight and obesity. We performed frequentist random-effect network meta-analyses to summarise the evidence and applied the Grading of Recommendations Assessment, Development, and Evaluation frameworks to rate the certainty of evidence, calculate the absolute effects, categorise interventions, and present the findings. The study was registered with PROSPERO, CRD 42021245678. FINDINGS: 14 605 citations were identified by our search, of which 143 eligible trials enrolled 49 810 participants. Except for levocarnitine, all drugs lowered bodyweight compared with lifestyle modification alone; all subsequent numbers refer to comparisons with lifestyle modification. High to moderate certainty evidence established phentermine-topiramate as the most effective in lowering weight (odds ratio [OR] of ≥5% weight reduction 8·02, 95% CI 5·24 to 12·27; mean difference [MD] of percentage bodyweight change -7·97, 95% CI -9·28 to -6·66) followed by GLP-1 receptor agonists (OR 6·33, 95% CI 5·00 to 8·00; MD -5·76, 95% CI -6·30 to -5·21). Naltrexone-bupropion (OR 2·69, 95% CI 2·11 to 3·43), phentermine-topiramate (2·40, 1·69 to 3·42), GLP-1 receptor agonists (2·17, 1·71 to 2·77), and orlistat (1·72, 1·44 to 2·05) were associated with increased adverse events leading to drug discontinuation. In a post-hoc analysis, semaglutide, a GLP-1 receptor agonist, showed substantially larger benefits than other drugs with a similar risk of adverse events as other drugs for both likelihood of weight loss of 5% or more (OR 9·82, 95% CI 7·09 to 13·61) and percentage bodyweight change (MD -11·41, 95% CI -12·54 to -10·27). INTERPRETATION: In adults with overweight and obesity, phentermine-topiramate and GLP-1 receptor agonists proved the best drugs in reducing weight; of the GLP-1 agonists, semaglutide might be the most effective. FUNDING: 1.3.5 Project for Disciplines of Excellence, West China Hospital, Sichuan University.
Sujet(s)
Agents antiobésité/administration et posologie , Obésité/traitement médicamenteux , Surpoids/traitement médicamenteux , Perte de poids/effets des médicaments et des substances chimiques , Adulte , Agents antiobésité/effets indésirables , Humains , Méta-analyse en réseau , Essais contrôlés randomisés comme sujet , Résultat thérapeutiqueRÉSUMÉ
Transdermal drug delivery (TDD) has recently emerged as an effective alternative to oral and injection administration because of its less invasiveness, low rejection rate, and excellent ease of administration. TDD has made an important contribution to medical practice such as diabetes, hemorrhoids, arthritis, migraine, and schizophrenia treatment, but has yet to fully achieve its potential in the treatment of obesity. Obesity has reached epidemic proportions globally and posed a significant threat to human health. Various approaches, including oral and injection administration have widely been used in clinical setting for obesity treatment. However, these traditional options remain ineffective and inconvenient, and carry risks of adverse effects. Therefore, alternative and advanced drug delivery strategies with higher efficacy and less toxicity such as TDD are urgently required for obesity treatment. This review summarizes current TDD technology, and the main anti-obesity drug delivery system. This review also provides insights into various anti-obesity drugs under study with a focus on the recent developments of TDD system for enhanced anti-obesity drug delivery. Although most of presented studies stay in animal stage, the application of TDD in anti-obesity drugs would have a significant impact on bringing safe and effective therapies to obese patients in the future.
