Phase I clinical trial of HC-1119 soft capsule in Chinese healthy adult male subjects: Pharmacokinetics and safety of single-dose proportionality and effects of food.

The Prostate Pub Date : 2022-02-01 Epub Date: 2021-11-22 DOI:10.1002/pros.24271

Haiping Ma, Weidong Xu, Jin Ni, Naping Zhao, Shouyan Tang, Song Li, Tingting Cai, Jianping Xiu, Xin Kang, Shen Gao, Li Zhang, Tie Zhou

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引用次数: 3

Abstract

Background: Preclinical studies showed that HC-1119, a deuterated version of enzalutamide, could competitively inhibit androgen binding to androgen receptor by blocking the transmission of androgen receptor signaling pathway as enzalutamide, inducing apoptosis of prostate cancer cells and reducing the proliferation of prostate cancer cells. Animal pharmacokinetic studies also show that deuterization of enzalutamide as HC-1119 could retain the basic properties of mother drug, increases the stability of compounds to metabolic enzymes and the drug exposure in vivo, prolong the half-life and reduce the production of metabolites, which may lead to a better efficacy and safety of HC-1119 compared with enzalutamide.

Methods: To evaluate the pharmacokinetics and safety of HC-1119 and the effects of food on pharmacokinetics in healthy adult Chinese men after single-dose administration of HC-1119. A total of 47 Chinese healthy adult male subjects received HC-1119 soft capsule at a single oral dose of 40, 80, or 160 mg followed on fasting or 160 mg after high-fat meal respectively. HC-1119 prototype and its metabolites M1 and M2 in plasma were collected individually in a total 23 time points. Pharmacokinetics were determined by sensitive LC/MS/MS for dose-proportionality study.

Results: In subjects taking HC-1119 soft capsules on fasting, C_max of HC-1119 prototype increased dose-dependently. Either C_max and AUC_0-∞ of M1 or C_max of M2 showed statistically significant difference. Dose-proportionality evaluation showed linear pharmacokinetic characteristics in C_max of HC-1119 prototype, C_max and AUC_0-∞ of M2 in dose range of 40-160 mg. C_max of HC-1119 was significantly different between the two groups as 160 mg HC-1119 on fasting or after a high-fat diet respectively, while the other parameter were not. HC-1119 and its metabolites M1 and M2 showed a linear dynamic trend.

Conclusions: HC-1119 is expected to have lower clinical dose than the similar drug enzalutamide. The absorption of HC-1119 and the main pharmacokinetic parameters of HC-1119 and its metabolites M1 and M2 were not affected by high-fat diet. The clinical application of HC-1119 soft capsule in the later stage can be recommended for both fasting and postprandial. The safety and tolerance were good in this population.

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HC-1119软胶囊在中国健康成年男性受试者体内的I期临床试验:药代动力学、安全性、单剂量比例及食用效果。

背景:临床前研究表明，HC-1119作为enzalutamide的氘化版本，通过阻断雄激素受体信号通路的传递，竞争性地抑制雄激素与雄激素受体的结合，诱导前列腺癌细胞凋亡，减少前列腺癌细胞的增殖。动物药代动力学研究也表明，将恩杂鲁胺氘化为HC-1119后，可以保留母药的基本性质，增加化合物对代谢酶的稳定性和药物在体内的暴露，延长半衰期，减少代谢物的产生，这可能导致HC-1119比恩杂鲁胺具有更好的疗效和安全性。方法:评价单次给药后HC-1119在中国健康成年男性体内的药代动力学和安全性，以及食物对其药代动力学的影响。共有47名中国健康成年男性受试者分别在禁食和高脂肪餐后分别口服40、80或160 mg的HC-1119软胶囊。在23个时间点分别采集HC-1119原型及其血浆代谢产物M1和M2。采用高效液相色谱/质谱/质谱法测定药代动力学，进行剂量比例研究。结果:空腹服用HC-1119软胶囊后，HC-1119原型体Cmax呈剂量依赖性增加。无论是M1的Cmax和AUC0-∞，还是M2的Cmax，差异均有统计学意义。剂量比例评价显示HC-1119原型药Cmax、M2的Cmax和AUC0-∞在40 ~ 160 mg剂量范围内呈线性药代动力学特征。在160 mg HC-1119空腹和高脂饮食后两组之间，HC-1119的Cmax差异有统计学意义，其他参数无统计学意义。HC-1119及其代谢产物M1、M2呈线性动态趋势。结论:HC-1119的临床剂量有望低于同类药物恩杂鲁胺。高脂饮食对HC-1119的吸收及主要药动学参数及其代谢产物M1、M2均无影响。HC-1119软胶囊的后期临床应用可推荐空腹和餐后使用。该人群安全性和耐受性良好。

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The Prostate

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