Non-clinical and first-in-human characterization of ECC5004/AZD5004, a novel once-daily, oral small-molecule GLP-1 receptor agonist

IF 5.4 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetes, Obesity & Metabolism Pub Date : 2024-11-04 DOI:10.1111/dom.16047

Amina Z. Haggag MD, Jianfeng Xu MD, Laurie Butcher MSc, Sandra Pagnussat MD, Graeme Davies PhD, Sara Lundqvist MSc, Wenyu Wang PhD, Natalie Van Zuydam PhD, Karin Nelander PhD, Aruni Jha PhD, Hongtao Yu PhD, Alessandro Boianelli PhD, Bosse Lindmark MSc, Anna Ollerstam PhD, Xuefeng Sun PhD, Fan Wang MSc, Xiaoliang Pan MSc, Haihui Liu MSc, Wengang Chen PhD, Jianfeng Xu PhD, Kristina Wallenius PhD, Jingye Zhou PhD

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Abstract

Aims

GLP-1 receptor agonists (GLP-1 RAs) are proven therapies for type 2 diabetes mellitus (T2DM) and overweight or obesity. We performed non-clinical and first-in-human (FIH) evaluation of ECC5004/AZD5004, an oral small-molecule GLP-1 RA.

Materials and Methods

ECC5004 was profiled in cell lines overexpressing human GLP-1R, in glucose-stimulated insulin secretion (GSIS) assays in a human β-cell line and non-human primates (NHPs). To evaluate safety, ECC5004 was orally administered to NHPs for 9 months and a phase I, double-blind, placebo-controlled FIH study was conducted. This study evaluated single doses of ECC5004 (1–300 mg) in healthy volunteers, and multiple daily doses (5, 10, 30 and 50 mg) in patients with T2DM for 28 days.

Results

ECC5004 bound to the hGLP-1R (IC₅₀ = 2.4 nM) augmented cAMP signalling without β-arrestin-2 recruitment or receptor internalization. ECC5004 potentiated GSIS in both EndoC-βH5 cells (EC₅₀ = 5.9 nM) and in vivo in NHPs (EC₅₀ = 0.022 nM). Dose-dependent body weight changes compared to control were seen in the 9-month NHP toxicity study. In the first-in-human study, ECC5004 was well tolerated with no serious adverse events. Dose-dependent reductions in glucose and body weight were observed with a dose-proportional exposure at doses ≥25 mg.

Conclusion

ECC5004 engaged the GLP-1R across the therapeutic dose range tested and had a safety and tolerability profile consistent with other GLP-1 RAs, along with a pharmacokinetic profile compatible with once-daily oral dosing. These data support continued development of ECC5004 as a potential therapy for T2DM and overweight or obesity. Clinical trial registration: NCT05654831.

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ECC5004/AZD5004--一种新型的每日一次口服小分子 GLP-1 受体激动剂--的非临床和首次人体试验表征。

目的：GLP-1受体激动剂（GLP-1 RAs）是治疗2型糖尿病（T2DM）和超重或肥胖症的行之有效的疗法。我们对口服小分子 GLP-1 RA ECC5004/AZD5004 进行了非临床和首次人体（FIH）评估：在过表达人 GLP-1R 的细胞系、人 β 细胞系和非人灵长类动物（NHPs）的葡萄糖刺激胰岛素分泌（GSIS）试验中对 ECC5004 进行了分析。为评估安全性，对非人灵长类动物口服了 9 个月的 ECC5004，并开展了一项 I 期、双盲、安慰剂对照 FIH 研究。该研究评估了健康志愿者服用单剂量 ECC5004（1-300 毫克）和 T2DM 患者服用多日剂量 ECC5004（5、10、30 和 50 毫克）达 28 天的情况：结果：ECC5004与hGLP-1R结合（IC50 = 2.4 nM）可增强cAMP信号传导，但没有β-restin-2招募或受体内化。ECC5004 在 EndoC-βH5 细胞（EC50 = 5.9 nM）和 NHPs 体内（EC50 = 0.022 nM）中都能增强 GSIS。在为期 9 个月的 NHP 毒性研究中，与对照组相比，出现了剂量依赖性体重变化。在首次人体试验中，ECC5004的耐受性良好，未出现严重不良反应。在剂量≥25毫克时，观察到葡萄糖和体重的减少与剂量成正比：结论：ECC5004在测试的治疗剂量范围内都能激活GLP-1R，其安全性和耐受性与其他GLP-1 RAs一致，药代动力学特征与每日一次口服剂量相符。这些数据支持继续开发 ECC5004 作为治疗 T2DM 和超重或肥胖症的潜在疗法：临床试验注册：NCT05654831。

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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.