Evaluation of an oral small-molecule glucagon-like peptide-1 receptor agonist, lotiglipron, for type 2 diabetes and obesity: A dose-ranging, phase 2, randomized, placebo-controlled study

IF 5.7 2区医学 Q1 ENDOCRINOLOGY & METABOLISM Diabetes, Obesity & Metabolism Pub Date : 2024-10-16 DOI:10.1111/dom.16005

Neeta B. Amin PharmD, Robert Frederich MD, Nikolaos Tsamandouras PhD, Amina Z. Haggag MD, Tilman Schuster PhD, Witold Zmuda MD, Alexandra Palmer BSc, Szilard Vasas MD, Gina Buckley MT, Timothy R. Smith MD, Sarah J. DuBrava MS, Qi Zhu MD, Margot Johnson MD

{"title":"Evaluation of an oral small-molecule glucagon-like peptide-1 receptor agonist, lotiglipron, for type 2 diabetes and obesity: A dose-ranging, phase 2, randomized, placebo-controlled study","authors":"Neeta B. Amin PharmD, Robert Frederich MD, Nikolaos Tsamandouras PhD, Amina Z. Haggag MD, Tilman Schuster PhD, Witold Zmuda MD, Alexandra Palmer BSc, Szilard Vasas MD, Gina Buckley MT, Timothy R. Smith MD, Sarah J. DuBrava MS, Qi Zhu MD, Margot Johnson MD","doi":"10.1111/dom.16005","DOIUrl":null,"url":null,"abstract":"<div>\n \n \n <section>\n \n <h3> Aim</h3>\n \n <p>The aim was to investigate the effects of lotiglipron, a once-daily, oral small-molecule glucagon-like peptide-1 (GLP-1) receptor agonist, in participants with type 2 diabetes (T2D) or obesity.</p>\n </section>\n \n <section>\n \n <h3> Materials and Methods</h3>\n \n <p>A phase 2, randomized, double-blind, placebo-controlled, dose-ranging study investigated the efficacy and safety of lotiglipron. The study was terminated early for safety reasons after routine data and monitoring review. The planned analyses for the end points were modified prior to unblinding the study.</p>\n </section>\n \n <section>\n \n <h3> Results</h3>\n \n <p>In total, 901 participants were treated with at least one dose of the study drug (T2D cohort: <i>n</i> = 512, obesity cohort: <i>n</i> = 389). Although the majority of participants who were randomly assigned to higher doses did not reach their target maintenance dose, statistically significant changes in HbA1c and body weight were observed. In the T2D cohort, reductions in HbA1c were observed across all lotiglipron doses at week 16 (<i>p</i> < 0.0001), with least squares mean decreases up to −1.44% (90% confidence interval [CI]: −1.63, −1.26) (lotiglipron 80 mg), versus placebo, −0.07% (90% CI: −0.25, 0.11). In the obesity cohort, decreases in body weight were observed across all lotiglipron doses at week 20 (<i>p</i> < 0.01), up to −7.47% (90% CI: −8.50, −6.43) (lotiglipron 200 mg, five-step titration), versus placebo, −1.84% (90% CI: −2.85, −0.83). Across cohorts, the most frequently reported treatment-emergent adverse events were gastrointestinal related (most mild to moderate severity), with nausea being the most common (ranging from 4% [placebo] to 28.8% [80 mg] in the T2D cohort and 12.5% [placebo] to 60.6% [200 mg, four-step titration] in the obesity cohort). Transaminase elevations were observed in a subset of participants (6.6% and 6.0% of participants on lotiglipron in the T2D and obesity cohorts, respectively, compared with 1.6% on placebo in the obesity cohort).</p>\n </section>\n \n <section>\n \n <h3> Conclusions</h3>\n \n <p>The efficacy (HbA1c and/or body weight) of a range of lotiglipron doses was demonstrated in T2D and obesity cohorts. The safety profile was largely consistent with what has been previously known about the mechanism of action. Our results are unique in reporting elevations in liver transaminases in a subset of participants treated with lotiglipron, with attempts to identify the at-risk population unsuccessful and therefore clinical development of lotiglipron terminated.</p>\n </section>\n \n <section>\n \n <h3> ClinicalTrials.gov</h3>\n \n <p>NCT05579977.</p>\n </section>\n </div>","PeriodicalId":158,"journal":{"name":"Diabetes, Obesity & Metabolism","volume":"27 1","pages":"215-227"},"PeriodicalIF":5.7000,"publicationDate":"2024-10-16","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11618248/pdf/","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Diabetes, Obesity & Metabolism","FirstCategoryId":"3","ListUrlMain":"https://dom-pubs.onlinelibrary.wiley.com/doi/10.1111/dom.16005","RegionNum":2,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"ENDOCRINOLOGY & METABOLISM","Score":null,"Total":0}

引用次数: 0

Abstract

Aim

The aim was to investigate the effects of lotiglipron, a once-daily, oral small-molecule glucagon-like peptide-1 (GLP-1) receptor agonist, in participants with type 2 diabetes (T2D) or obesity.

Materials and Methods

A phase 2, randomized, double-blind, placebo-controlled, dose-ranging study investigated the efficacy and safety of lotiglipron. The study was terminated early for safety reasons after routine data and monitoring review. The planned analyses for the end points were modified prior to unblinding the study.

Results

In total, 901 participants were treated with at least one dose of the study drug (T2D cohort: n = 512, obesity cohort: n = 389). Although the majority of participants who were randomly assigned to higher doses did not reach their target maintenance dose, statistically significant changes in HbA1c and body weight were observed. In the T2D cohort, reductions in HbA1c were observed across all lotiglipron doses at week 16 (p < 0.0001), with least squares mean decreases up to −1.44% (90% confidence interval [CI]: −1.63, −1.26) (lotiglipron 80 mg), versus placebo, −0.07% (90% CI: −0.25, 0.11). In the obesity cohort, decreases in body weight were observed across all lotiglipron doses at week 20 (p < 0.01), up to −7.47% (90% CI: −8.50, −6.43) (lotiglipron 200 mg, five-step titration), versus placebo, −1.84% (90% CI: −2.85, −0.83). Across cohorts, the most frequently reported treatment-emergent adverse events were gastrointestinal related (most mild to moderate severity), with nausea being the most common (ranging from 4% [placebo] to 28.8% [80 mg] in the T2D cohort and 12.5% [placebo] to 60.6% [200 mg, four-step titration] in the obesity cohort). Transaminase elevations were observed in a subset of participants (6.6% and 6.0% of participants on lotiglipron in the T2D and obesity cohorts, respectively, compared with 1.6% on placebo in the obesity cohort).

Conclusions

The efficacy (HbA1c and/or body weight) of a range of lotiglipron doses was demonstrated in T2D and obesity cohorts. The safety profile was largely consistent with what has been previously known about the mechanism of action. Our results are unique in reporting elevations in liver transaminases in a subset of participants treated with lotiglipron, with attempts to identify the at-risk population unsuccessful and therefore clinical development of lotiglipron terminated.

ClinicalTrials.gov

NCT05579977.

Abstract Image

查看原文

微信好友朋友圈 QQ好友复制链接

本刊更多论文

评估口服小分子胰高血糖素样肽-1 受体激动剂 Lotiglipron 治疗 2 型糖尿病和肥胖症的效果：一项剂量不等的 2 期随机安慰剂对照研究。

目的：该研究旨在探讨每日一次口服小分子胰高血糖素样肽-1（GLP-1）受体激动剂洛替利普隆对2型糖尿病（T2D）或肥胖症患者的作用：一项 2 期随机、双盲、安慰剂对照、剂量范围研究调查了洛替利普隆的疗效和安全性。该研究在常规数据和监测审查后因安全性原因提前结束。在解除研究盲点之前，对终点的计划分析进行了修改：共有901名参与者接受了至少一剂研究药物的治疗（T2D队列：n = 512，肥胖队列：n = 389）。虽然大多数被随机分配到较高剂量的参与者没有达到目标维持剂量，但在 HbA1c 和体重方面观察到了统计学意义上的显著变化。在 T2D 组群中，所有洛替利普隆剂量在第 16 周均可观察到 HbA1c 下降（p 结论）：在 T2D 和肥胖人群中，一系列 lotiglipron 剂量的疗效（HbA1c 和/或体重）均已得到证实。其安全性与之前已知的作用机制基本一致。我们的研究结果是独一无二的，它报告了接受洛替利普隆治疗的部分参与者肝脏转氨酶升高，而确定高危人群的尝试并不成功，因此终止了洛替利普隆的临床开发：GOV：NCT05579977。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文去求助

来源期刊

Diabetes, Obesity & Metabolism 医学-内分泌学与代谢

CiteScore

10.90

自引率

6.90%

发文量

319

审稿时长

3-8 weeks

期刊介绍： Diabetes, Obesity and Metabolism is primarily a journal of clinical and experimental pharmacology and therapeutics covering the interrelated areas of diabetes, obesity and metabolism. The journal prioritises high-quality original research that reports on the effects of new or existing therapies, including dietary, exercise and lifestyle (non-pharmacological) interventions, in any aspect of metabolic and endocrine disease, either in humans or animal and cellular systems. ‘Metabolism’ may relate to lipids, bone and drug metabolism, or broader aspects of endocrine dysfunction. Preclinical pharmacology, pharmacokinetic studies, meta-analyses and those addressing drug safety and tolerability are also highly suitable for publication in this journal. Original research may be published as a main paper or as a research letter.