Smith William B, Nguyen David, Clough Timothy, Schofield Jül, Kagan Mark R, Kompa Jill, He YanLing, Maratos-Flier Eleftheria, Jamontt Joanna, Vong Linh, Schwartzkopf Chad D, Layne Joseph D, Usera Aimee R, O'Donnell Christopher J, Heldwein Kurt A, Streeper Ryan S, Goldfine Allison B
Alliance for Multispecialty Research, LLC, Knoxville, TN 37909, USA.
Altasciences Clinical Los Angeles, Inc., Cypress, CA 90630, USA.
J Clin Endocrinol Metab. 2025 Feb 18;110(3):771-786. doi: 10.1210/clinem/dgae550.
Growth differentiation factor 15 (GDF15), a divergent member of the TGF-β superfamily, signals via the hindbrain glial-derived neurotrophic factor receptor alpha-like and rearranged during transfection receptor co-receptor (GFRAL-RET) complex. In nonclinical species, GDF15 is a potent anorexigen leading to substantial weight loss. MBL949 is a half-life extended recombinant human GDF15 dimer.
MBL949 was evaluated in multiple nonclinical species, and then in humans, in 2 randomized and placebo-controlled clinical trials. In the phase 1, first-in-human, single ascending dose trial, MBL949 or placebo was injected subcutaneously to overweight and obese healthy volunteers (n = 65) at doses ranging from 0.03 to 20 mg. In phase 2, MBL949 or placebo was administered subcutaneously every other week for a total of 8 doses to obese participants (n = 126) in 5 different dose regimens predicted to be efficacious based on data from the phase 1 trial.
In nonclinical species, MBL949 was generally safe and effective with reduced food intake and body weight in mice, rats, dogs, and monkeys. Weight loss was primarily from reduced fat, and metabolic endpoints improved. A single ascending dose study in overweight or obese healthy adults demonstrated mean terminal half-life of 18 to 22 days and evidence of weight loss at the higher doses. In the phase 2, weight loss was minimal following biweekly dosing of MBL949 for 14 weeks. MBL949 was safe and generally tolerated in humans over the dose range tested, adverse events of the gastrointestinal system were the most frequent observed.
The prolonged half-life of MBL949 supports biweekly dosing in patients. MBL949 had an acceptable safety profile. The robust weight loss observed in nonclinical species did not translate to weight loss efficacy in humans.
生长分化因子15(GDF15)是转化生长因子-β(TGF-β)超家族的一个不同成员,通过后脑胶质细胞源性神经营养因子受体α样分子和转染期间重排受体共同受体(GFRAL-RET)复合物发出信号。在非临床物种中,GDF15是一种强效的食欲抑制剂,可导致显著体重减轻。MBL949是一种半衰期延长的重组人GDF15二聚体。
在多项非临床物种中对MBL949进行了评估,然后在两项随机、安慰剂对照的临床试验中对人类进行了评估。在1期首次人体单剂量递增试验中,将MBL949或安慰剂以0.03至20毫克的剂量皮下注射给超重和肥胖的健康志愿者(n = 65)。在2期试验中,根据1期试验的数据,以5种不同的预计有效剂量方案,每隔一周皮下注射一次MBL949或安慰剂,共8剂,给药对象为肥胖参与者(n = 126)。
在非临床物种中,MBL949总体上安全有效,可使小鼠、大鼠、狗和猴子的食物摄入量和体重降低。体重减轻主要源于脂肪减少,代谢指标得到改善。一项针对超重或肥胖健康成年人的单剂量递增研究表明,平均终末半衰期为18至22天,且在较高剂量下有体重减轻的迹象。在2期试验中,每两周给药一次MBL949,持续14周后体重减轻甚微。在测试的剂量范围内,MBL949在人体中安全且一般耐受性良好,最常观察到的不良事件是胃肠道系统的不良事件。
MBL949延长的半衰期支持每两周给患者给药一次。MBL949具有可接受的安全性。在非临床物种中观察到的显著体重减轻并未转化为在人体中的减肥疗效。
