ACD856, a novel positive allosteric modulator of Trk receptors, single ascending doses in healthy subjects: Safety and pharmacokinetics.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
ACS Applied Bio Materials Pub Date : 2024-05-01 Epub Date: 2024-02-14 DOI:10.1007/s00228-024-03645-1
Boel Nilsson, Johan Bylund, Magnus M Halldin, Matthias Rother, Erik Rein-Hedin, Kristin Önnestam, Märta Segerdahl
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引用次数: 0

Abstract

Purpose: AlzeCure Pharma AB is developing novel positive allosteric modulators of Trk-receptors for treatment of Alzheimer's disease, depression, other psychiatric conditions and other disorders where cognition is impaired. The preceding candidate drug ACD855 was shown to have a too long half-life in humans to allow further development. To de-risk the development of the follow-up compound ACD856, the oral single ascending dose study of ACD856 in humans was preceded by an intravenous microdose study, assessing the elimination half-life in plasma.

Methods: A phase 0 study with a microdose of ACD856 (0.100 mg), was conducted in six healthy male subjects all receiving ACD856. Sequentially, a randomized, placebo-controlled, double-blind Phase I single ascending oral dose study (1 - 150 mg) was conducted, including 56 healthy subjects. Both studies assessed the safety and tolerability, as well as the PK properties of ACD856 after single dose intravenous and oral administration.

Results: ACD856 was well tolerated with no treatment emergent, or dose related adverse events or other safety assessments. In the microdose study, ACD856 exhibited a bi-exponential plasma decline, low distribution volume, low plasma clearance with a half-life of approximately 20 hours. Orally, ACD856 exhibited rapid absorption, an almost complete bioavailability and a dose proportional increase in exposure. While the Cmax was lowered and delayed by food intake, the effect on plasma half-life and the overall bioavailability was low. No renal elimination of ACD856 was detected.

Conclusion: The prediction proved accurate demonstrating the value of conducting a microdose study prior to ascending dose studies.

Trial registration: NCT05783830 March 24, 2023 (microdose study, retrospectively registered) and NCT05077631 October 14, 2021 (single ascending dose study).

Abstract Image

ACD856是一种新型的Trk受体正异位调节剂,在健康受试者中使用单次升剂量:安全性和药代动力学。
目的:AlzeCure Pharma AB 公司正在开发新型 Trk 受体正异位调节剂,用于治疗阿尔茨海默病、抑郁症、其他精神疾病和其他认知障碍疾病。之前的候选药物 ACD855 在人体中的半衰期过长,无法进一步开发。为了降低后续化合物 ACD856 的开发风险,在对 ACD856 进行口服单升剂量人体研究之前,先进行了一项静脉微剂量研究,以评估其在血浆中的消除半衰期:在六名健康男性受试者中进行了微剂量 ACD856(0.100 毫克)的 0 期研究,所有受试者都接受了 ACD856。随后,对 56 名健康受试者进行了随机、安慰剂对照、双盲 I 期单次递增口服剂量研究(1 - 150 毫克)。两项研究均评估了单剂量静脉注射和口服 ACD856 的安全性、耐受性和 PK 特性:结果:ACD856的耐受性良好,没有出现治疗突发、与剂量相关的不良事件或其他安全性评估。在微剂量研究中,ACD856的血浆呈双指数下降,分布容积低,血浆清除率低,半衰期约为20小时。口服 ACD856 可快速吸收,生物利用度几乎完全,暴露量的增加与剂量成正比。虽然摄入食物会降低 Cmax 值并使其延迟,但对血浆半衰期和总体生物利用度的影响较小。未发现 ACD856 经肾脏排出:预测结果准确无误,证明了在升剂量研究之前进行微剂量研究的价值:试验注册:NCT05783830 2023年3月24日(微剂量研究,回顾性注册)和NCT05077631 2021年10月14日(单次升剂量研究)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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