Early Clinical Development, IMED Biotech Unit, AstraZeneca, Gothenburg, Sweden.
Department of Molecular and Clinical Medicine, Institute of Medicine, Sahlgrenska Academy at the University of Gothenburg, Gothenburg, Sweden.
Br J Clin Pharmacol. 2019 Apr;85(4):762-770. doi: 10.1111/bcp.13855. Epub 2019 Feb 18.
Myeloperoxidase activity can contribute to impaired vascular endothelial function and fibrosis in chronic inflammation-related cardiovascular disease. Here, we investigated the safety, tolerability and pharmacokinetics of the myeloperoxidase inhibitor, AZD4831.
In this randomized, single-blind, placebo-controlled, phase I, first-in-human study, healthy men in five sequential cohorts were randomized 3:1 to receive a single oral dose of AZD4831 (5, 15, 45, 135 or 405 mg) or placebo, after overnight fasting. After at least 7 days' washout, one cohort additionally received AZD4831 45 mg after a high-calorie meal.
Forty men participated in the study (eight per cohort: AZD4831, n = 6; placebo, n = 2). AZD4831 distributed rapidly into plasma, with a half-life of 38.2-50.0 hours. The area under the plasma concentration-time curve (AUC) increased proportionally with dose (AUC slope estimate 1.060; 95% confidence interval [CI] 0.9943, 1.127). Increases in maximum plasma concentration were slightly more than dose proportional (slope estimate 1.201; 95% CI 1.071, 1.332). Food intake reduced AZD4831 absorption rate but did not substantially affect overall exposure or plasma half-life (n = 4). Serum uric acid concentrations decreased by 71.77 (95% CI 29.15, 114.39) and 84.42 (58.90, 109.94) μmol L with AZD4831 135 mg and 405 mg, respectively. Maculopapular rash (moderate intensity) occurred in 4/30 participants receiving AZD4831 (13.3%). No other safety concerns were identified.
AZD4831 was generally well tolerated, rapidly absorbed, had a long plasma half-life and lowered uric acid concentrations after single oral doses in healthy men. These findings support the further clinical development of AZD4831.
髓过氧化物酶活性可导致慢性炎症相关心血管疾病中的血管内皮功能障碍和纤维化。在此,我们研究了髓过氧化物酶抑制剂 AZD4831 的安全性、耐受性和药代动力学。
在这项随机、单盲、安慰剂对照、I 期、首次人体研究中,连续 5 个队列的健康男性在禁食过夜后,按照 3:1 的比例随机接受单次口服 AZD4831(5、15、45、135 或 405mg)或安慰剂治疗。至少洗脱 7 天后,一个队列在高卡路里餐后额外接受 AZD4831 45mg。
40 名男性参加了这项研究(每个队列 8 人:AZD4831,n=6;安慰剂,n=2)。AZD4831 迅速分布到血浆中,半衰期为 38.2-50.0 小时。血浆浓度-时间曲线下面积(AUC)与剂量呈比例增加(AUC 斜率估计值 1.060;95%置信区间 [CI] 0.9943,1.127)。最大血浆浓度的增加略高于剂量比例(斜率估计值 1.201;95% CI 1.071,1.332)。食物摄入降低了 AZD4831 的吸收速率,但并未实质性影响总体暴露或血浆半衰期(n=4)。血清尿酸浓度分别下降 71.77(95% CI 29.15,114.39)和 84.42(58.90,109.94)μmol/L,AZD4831 的剂量分别为 135mg 和 405mg。接受 AZD4831 治疗的 30 名参与者中有 4 名(13.3%)出现斑丘疹(中度强度)。未发现其他安全性问题。
AZD4831 在健康男性单次口服后,总体耐受性良好,吸收迅速,血浆半衰期长,降低尿酸浓度。这些发现支持 AZD4831 的进一步临床开发。
