Pharmacokinetics, Safety, and Tolerability of Tenapanor in Healthy Chinese and Caucasian Volunteers: A Randomized, Open-Label, Single-Center, Placebo-Controlled Phase 1 Study

IF 2.2 4区 医学 Q2 MEDICINE, GENERAL & INTERNAL International Journal of Clinical Practice Pub Date : 2024-03-06 DOI:10.1155/2024/1386980
Gang Yuan, Yili Chen, Li Li, Xin Wang, Gang Wei, Jiawei Zeng, Ai-Min Hui, Yueyun Jiang, Han Zhao, Lei Diao, Yongchun Zhou, Yinglian Xiao, Minhu Chen
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Abstract

Background. Tenapanor is a locally acting selective sodium-hydrogen exchanger 3 inhibitor with the potential to treat sodium/phosphorus and fluid overload in various cardiac-renal diseases, which has been approved for constipation-predominant irritable bowel syndrome in the US. The pharmacokinetics (PK) of tenapanor and its metabolite tenapanor-M1 (AZ13792925), as well as the safety and tolerability of tenapanor, were investigated in healthy Chinese and Caucasian subjects. Methods. This randomized, open-label, single-center, placebo-controlled phase 1 study (https://www.chinadrugtrials.org.cn; CTR20201783) enrolled Chinese and Caucasian healthy volunteers into 4 parallel cohorts (3 cohorts for Chinese subjects, 1 cohort for Caucasian subjects). In each cohort, 15 subjects were expected to be included and received oral tenapanor (10 or 30 mg as single dose, or 50 mg as a single dose followed by a twice-daily repeated dose from Day 5 to 11, with a single dose in the morning on Day 11) or placebo in a 4 : 1 ratio. Results. 59 healthy volunteers received tenapanor 10 mg (n = 12 Chinese), 30 mg (n = 12 Chinese), or 50 mg (n = 12 (Chinese), n = 11 (Caucasian)) or placebo (n = 12, 3 per cohort). After single and twice-daily repeated doses, tenapanor plasma concentrations were all below the limit of quantitation; tenapanor-M1 appeared slowly in plasma. In single-ascending dose evaluation (10 to 50 mg) of Chinese subjects, the mean Cmax, AUC0-t, and AUC0-∞ of tenapanor-M1 increased with increasing dose level, and AUC0-t increased approximately dose proportionally. The Cmax accumulation ratio was 1.55 to 6.92 after 50 mg repeated dose in Chinese and Caucasian subjects. Exposure to tenapanor-M1 was generally similar between the Chinese and Caucasian subjects. Tenapanor was generally well-tolerated and the safety profile was similar between the Chinese and Caucasian participants receiving tenapanor 50 mg, as measured by vital signs, physical and laboratory examination, 12-lead ECG, and adverse events. No serious adverse event or adverse event leading to withdrawal occurred. Conclusion. Tenapanor was well-tolerated, with similar PK and safety profiles between Chinese and Caucasian subjects. This trial is registered with CTR20201783.

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特纳帕诺在健康中国人和白种人志愿者中的药代动力学、安全性和耐受性:一项随机、开放标签、单中心、安慰剂对照的 1 期研究
背景。替那帕诺是一种局部作用的选择性钠-氢交换机 3 抑制剂,可用于治疗各种心肾疾病的钠/磷和体液超负荷,在美国已被批准用于治疗以便秘为主的肠易激综合征。研究人员在健康的中国人和白种人受试者中研究了替那潘诺及其代谢物替那潘诺-M1(AZ13792925)的药代动力学(PK)以及替那潘诺的安全性和耐受性。研究方法这项随机、开放标签、单中心、安慰剂对照的1期研究(https://www.chinadrugtrials.org.cn; CTR20201783)将中国和高加索健康志愿者分为4个平行队列(中国受试者3个队列,高加索受试者1个队列)。每个队列预计纳入 15 名受试者,受试者按 4:1 的比例口服替那潘诺(单次剂量 10 或 30 毫克,或单次剂量 50 毫克,然后从第 5 天到第 11 天每天重复服用两次,第 11 天早上服用一次)或安慰剂:1 的比例服用。研究结果59 名健康志愿者分别服用了替那潘诺 10 毫克(中国人 12 人)、30 毫克(中国人 12 人)或 50 毫克(中国人 12 人,白人 11 人)或安慰剂(12 人,每组 3 人)。单次和每日两次重复给药后,替那帕诺的血浆浓度均低于定量限;替那帕诺-M1在血浆中出现缓慢。在对中国受试者进行的单次递增剂量评估(10 至 50 毫克)中,替那帕诺-M1 的平均值、AUC0-t 和 AUC0-∞ 随着剂量的增加而增加,AUC0-t 的增加与剂量成正比。中国人和白种人重复服用 50 毫克后的蓄积比为 1.55 至 6.92。中国受试者和高加索受试者对替那帕诺-M1的暴露量大致相似。根据生命体征、体格和实验室检查、12导联心电图以及不良事件等指标,接受替那潘诺50毫克治疗的中国受试者和高加索受试者的耐受性和安全性基本相似。没有发生严重不良事件或导致停药的不良事件。结论替那帕诺耐受性良好,中国受试者和白种人受试者的PK和安全性相似。该试验的注册号为CTR20201783。
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来源期刊
CiteScore
5.30
自引率
0.00%
发文量
274
审稿时长
3-8 weeks
期刊介绍: IJCP is a general medical journal. IJCP gives special priority to work that has international appeal. IJCP publishes: Editorials. IJCP Editorials are commissioned. [Peer reviewed at the editor''s discretion] Perspectives. Most IJCP Perspectives are commissioned. Example. [Peer reviewed at the editor''s discretion] Study design and interpretation. Example. [Always peer reviewed] Original data from clinical investigations. In particular: Primary research papers from RCTs, observational studies, epidemiological studies; pre-specified sub-analyses; pooled analyses. [Always peer reviewed] Meta-analyses. [Always peer reviewed] Systematic reviews. From October 2009, special priority will be given to systematic reviews. [Always peer reviewed] Non-systematic/narrative reviews. From October 2009, reviews that are not systematic will be considered only if they include a discrete Methods section that must explicitly describe the authors'' approach. Special priority will, however, be given to systematic reviews. [Always peer reviewed] ''How to…'' papers. Example. [Always peer reviewed] Consensus statements. [Always peer reviewed] Short reports. [Always peer reviewed] Letters. [Peer reviewed at the editor''s discretion] International scope IJCP publishes work from investigators globally. Around 30% of IJCP articles list an author from the UK. Around 30% of IJCP articles list an author from the USA or Canada. Around 45% of IJCP articles list an author from a European country that is not the UK. Around 15% of articles published in IJCP list an author from a country in the Asia-Pacific region.
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