The Pharmacokinetics, Safety and Tolerability of Aclidinium Bromide 400 μg Administered by Inhalation as Single and Multiple (Twice Daily) Doses in Healthy Chinese Participants.

IF 2.7 3区医学 Q2 RESPIRATORY SYSTEM International Journal of Chronic Obstructive Pulmonary Disease Pub Date : 2023-11-27 eCollection Date: 2023-01-01 DOI:10.2147/COPD.S434588

Weimin Li, Sami Z Daoud, Roopa Trivedi, Pradeep B Lukka, Eulalia Jimenez, Eduard Molins, Catherine Stewart, Pranob Bharali, Esther Garcia-Gil

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Abstract

Purpose: To date, aclidinium pharmacokinetic (PK) studies have focused on Caucasian populations, and no data are available for Chinese populations. We aimed to characterize the PK and safety profile of aclidinium and its metabolites (LAS34823 and LAS34850) following single and multiple (twice-daily; BID) dosing in healthy Chinese participants, and to compare PK data between Chinese and Caucasian populations.

Materials and methods: In this Phase I, open-label study (NCT03276052), healthy participants from a single site in China received aclidinium bromide 400 µg via a dry powder inhaler. The Day 1 single dose was followed by a washout period of 96 hours. On Days 5 through 8, participants received BID doses.

Results: Twenty healthy Chinese participants, aged 18-45 years, were enrolled. Aclidinium absorption was rapid (median time to maximum concentration [t_max] 0.08 hours post-dose following single/multiple doses). LAS34823 had a similar median t_max of 0.08 hours, whereas LAS34850 t_max occurred later (median 2.50-3.00 hours). Aclidinium, LAS34823, and LAS34850 concentrations declined in a bi-phasic manner; geometric mean half-life was 13.5 hours (single dosing) and 21.4 hours (multiple dosing), while steady state was generally achieved after 5 days' continuous dosing. Area under the concentration-time curve during a dosage interval (AUC_τ) metabolite to parent ratios for LAS34823 were 2.6 (Day 1) and 2.9 (Day 9), while LAS34850 had ratios of 136.0 and 94.8, respectively. Aclidinium accumulation occurred after 5 days of BID dosing (LS mean accumulation ratio for AUC_τ Day 9/Day 1: 214.1% [90% CI, 176.5, 259.6]); LAS34823 accumulation was similar, while LAS34850 accumulation was lower. Between-participant exposure variability was moderate to high for aclidinium and LAS34823, and low for LAS34850.

Conclusion: Single and multiple doses of aclidinium were well tolerated in healthy Chinese participants. The safety profile of and exposure to aclidinium was consistent with previous studies conducted in Caucasian populations.

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中国健康受试者单次和多次(每日两次)吸入400 μg吖啶铵的药代动力学、安全性和耐受性

目的:迄今为止，吖啶啶药代动力学(PK)研究主要集中在高加索人群，没有针对中国人群的数据。我们的目的是在单次和多次(每日两次;并比较中国和高加索人群之间的PK数据。材料和方法:在这项I期开放标签研究(NCT03276052)中，来自中国单一地点的健康参与者通过干粉吸入器接受了400µg的溴化aclidinium。第1天单次给药后为96小时的洗脱期。在第5至8天，参与者接受BID剂量。结果:20名年龄在18-45岁的健康中国受试者入组。吖啶吸收迅速(单次/多次给药后中位时间至最大浓度[tmax]为0.08小时)。LAS34823的tmax中位数相似，为0.08小时，而LAS34850的tmax发生较晚(中位数为2.50-3.00小时)。Aclidinium、LAS34823和LAS34850浓度呈双相下降;几何平均半衰期为单次给药13.5小时，多次给药21.4小时，一般连续给药5天后达到稳定状态。剂量间隔(AUCτ)期间，LAS34823的代谢物与亲本比值分别为2.6(第1天)和2.9(第9天)，而LAS34850的代谢物与亲本比值分别为136.0和94.8。BID给药5天后发生吖啶积累(AUCτ第9天/第1天的LS平均积累比:214.1% [90% CI, 176.5, 259.6]);LAS34823积累量相似，而LAS34850积累量较低。受试者之间的暴露变异性对吖啶铵和LAS34823为中高，对LAS34850为低。结论:单剂量和多剂量的吖啶铵在中国健康受试者中耐受性良好。对吖啶铵的安全性和暴露与先前在高加索人群中进行的研究一致。

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来源期刊

International Journal of Chronic Obstructive Pulmonary Disease RESPIRATORY SYSTEM-

CiteScore

4.80

自引率

10.70%

发文量

372

审稿时长

16 weeks

期刊介绍： An international, peer-reviewed journal of therapeutics and pharmacology focusing on concise rapid reporting of clinical studies and reviews in COPD. Special focus will be given to the pathophysiological processes underlying the disease, intervention programs, patient focused education, and self management protocols. This journal is directed at specialists and healthcare professionals