AKR1C3 抑制剂 BAY1128688 的肝毒性:一项治疗子宫内膜异位症的提前终止的 IIa 期试验结果。
Hepatotoxicity of AKR1C3 Inhibitor BAY1128688: Findings from an Early Terminated Phase IIa Trial for the Treatment of Endometriosis.
机构信息
Pharmaceuticals, Bayer AG, Berlin, Germany.
Svelte® scientific GmbH, Berlin, Germany.
出版信息
Drugs R D. 2023 Sep;23(3):221-237. doi: 10.1007/s40268-023-00427-5. Epub 2023 Jul 9.
INTRODUCTION
BAY1128688 is a selective inhibitor of aldo-keto reductase family 1 member C3 (AKR1C3), an enzyme implicated in the pathology of endometriosis and other disorders. In vivo animal studies suggested a potential therapeutic application of BAY1128688 in treating endometriosis. Early clinical studies in healthy volunteers supported the start of phase IIa.
OBJECTIVE
This manuscript reports the results of a clinical trial (AKRENDO1) assessing the effects of BAY1128688 in adult premenopausal women with endometriosis-related pain symptoms over a 12-week treatment period.
METHODS
Participants in this placebo-controlled, multicenter phase IIa clinical trial (NCT03373422) were randomized into one of five BAY1128688 treatment groups: 3 mg once daily (OD), 10 mg OD, 30 mg OD, 30 mg twice daily (BID), 60 mg BID; or a placebo group. The efficacy, safety, and tolerability of BAY1128688 were investigated.
RESULTS
Dose-/exposure-dependent hepatotoxicity was observed following BAY1128688 treatment, characterized by elevations in serum alanine transferase (ALT) occurring at around 12 weeks of treatment and prompting premature trial termination. The reduced number of valid trial completers precludes conclusions regarding treatment efficacy. The pharmacokinetics and pharmacodynamics of BAY1128688 among participants with endometriosis were comparable with those previously found in healthy volunteers and were not predictive of the subsequent ALT elevations observed.
CONCLUSIONS
The hepatotoxicity of BAY1128688 observed in AKRENDO1 was not predicted by animal studies nor by studies in healthy volunteers. However, in vitro interactions of BAY1128688 with bile salt transporters indicated a potential risk factor for hepatotoxicity at higher doses. This highlights the importance of in vitro mechanistic and transporter interaction studies in the assessment of hepatoxicity risk and suggests further mechanistic understanding is required.
CLINICAL TRIAL REGISTRATION
NCT03373422 (date registered: November 23, 2017).
简介
BAY1128688 是醛酮还原酶家族 1 成员 C3(AKR1C3)的选择性抑制剂,该酶与子宫内膜异位症和其他疾病的病理有关。体内动物研究表明,BAY1128688 在治疗子宫内膜异位症方面具有潜在的治疗应用。早期在健康志愿者中的临床研究支持开始进行 IIa 期研究。
目的
本文报告了一项临床试验(AKRENDO1)的结果,该试验评估了 BAY1128688 在 12 周治疗期间对患有与子宫内膜异位症相关疼痛症状的绝经前成年女性的影响。
方法
这项安慰剂对照、多中心 IIa 期临床试验(NCT03373422)的参与者被随机分为五组 BAY1128688 治疗组之一:每天一次 3 毫克(OD)、每天一次 10 毫克(OD)、每天一次 30 毫克(OD)、每天两次 30 毫克(BID)、每天两次 60 毫克(BID);或安慰剂组。研究了 BAY1128688 的疗效、安全性和耐受性。
结果
在 BAY1128688 治疗后观察到剂量/暴露依赖性肝毒性,其特征为治疗约 12 周时血清丙氨酸转氨酶(ALT)升高,并促使试验提前终止。有效试验完成者人数减少,无法得出关于治疗效果的结论。子宫内膜异位症参与者的 BAY1128688 药代动力学和药效学与先前在健康志愿者中发现的相似,并且不能预测随后观察到的 ALT 升高。
结论
AKRENDO1 中观察到的 BAY1128688 肝毒性不能通过动物研究或健康志愿者研究预测。然而,BAY1128688 与胆汁盐转运体的体外相互作用表明,在较高剂量下存在肝毒性的潜在危险因素。这凸显了在评估肝毒性风险时进行体外机制和转运体相互作用研究的重要性,并表明需要进一步的机制理解。
临床试验注册
NCT03373422(注册日期:2017 年 11 月 23 日)。
Zotero 插件