Physiologically-based pharmacokinetic/pharmacodynamic modeling to predict tumor growth inhibition and the efficacious dose of selective estrogen receptor degraders in humans

IF 1.7 4区医学 Q3 PHARMACOLOGY & PHARMACY Biopharmaceutics & Drug Disposition Pub Date : 2023-04-27 DOI:10.1002/bdd.2358

Anjani Ganti, Sijia Yu, Danielle Sharpnack, Ellen Ingalla, Tom De Bruyn

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引用次数: 1

Abstract

GDC-9545 (giredestrant) is a highly potent, nonsteroidal, oral selective estrogen receptor antagonist and degrader that is being developed as a best-in-class drug candidate for early-stage and advanced drug-resistant breast cancer. GDC-9545 was designed to improve the poor absorption and metabolism of its predecessor GDC-0927, for which development was halted due to a high pill burden. This study aimed to develop physiologically-based pharmacokinetic/pharmacodynamic (PBPK-PD) models to characterize the relationships between oral exposure of GDC-9545 and GDC-0927 and tumor regression in HCI-013 tumor-bearing mice, and to translate these PK-PD relationships to a projected human efficacious dose by integrating clinical PK data. PBPK and Simeoni tumor growth inhibition (TGI) models were developed using the animal and human Simcyp V20 Simulator (Certara) and adequately described each compound's systemic drug concentrations and antitumor activity in the dose-ranging xenograft experiments in mice. The established PK-PD relationship was translated to a human efficacious dose by substituting mouse PK for human PK. PBPK input values for human clearance were predicted using allometry and in vitro in vivo extrapolation approaches and human volume of distribution was predicted from simple allometry or tissue composition equations. The integrated human PBPK-PD model was used to simulate TGI at clinically relevant doses. Translating the murine PBPK-PD relationship to a human efficacious dose projected a much lower efficacious dose for GDC-9545 than GDC-0927. Additional sensitivity analysis of key parameters in the PK-PD model demonstrated that the lower efficacious dose of GDC-9545 is a result of improvements in clearance and absorption. The presented PBPK-PD methodology can be applied to support lead optimization and clinical development of many drug candidates in discovery or early development programs.

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基于生理的药代动力学/药效学模型预测肿瘤生长抑制和选择性雌激素受体降解剂在人体中的有效剂量

GDC-9545 (giredestrant)是一种高效、非甾体、口服选择性雌激素受体拮抗剂和降解剂，正被开发为治疗早期和晚期耐药乳腺癌的同类最佳候选药物。GDC-9545旨在改善其前身GDC-0927的不良吸收和代谢，GDC-0927的开发因高药丸负担而停止。本研究旨在建立基于生理的药代动力学/药效学(PBPK-PD)模型，以表征口服GDC-9545和GDC-0927与HCI-013荷瘤小鼠肿瘤消退之间的关系，并通过整合临床PK数据将这些PK- pd关系转化为预计的人体有效剂量。使用动物和人类Simcyp V20模拟器(Certara)建立PBPK和Simeoni肿瘤生长抑制(TGI)模型，并充分描述了每种化合物在小鼠剂量范围异种移植实验中的全身药物浓度和抗肿瘤活性。通过将小鼠PK代入人体PK，将已建立的PK- pd关系转化为人体有效剂量。利用异速测定法和体外体内外推法预测人体清除率的PBPK输入值，并通过简单的异速测定法或组织组成方程预测人体体积分布。采用人PBPK-PD综合模型模拟临床相关剂量下的TGI。将小鼠PBPK-PD关系转化为人体有效剂量，预测GDC-9545的有效剂量远低于GDC-0927。另外对PK-PD模型关键参数的敏感性分析表明，GDC-9545有效剂量的降低是由于清除和吸收的改善。提出的PBPK-PD方法可以应用于支持先导物优化和许多候选药物在发现或早期开发项目的临床开发。

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来源期刊

Biopharmaceutics & Drug Disposition 医学-药学

CiteScore

3.60

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： Biopharmaceutics & Drug Dispositionpublishes original review articles, short communications, and reports in biopharmaceutics, drug disposition, pharmacokinetics and pharmacodynamics, especially those that have a direct relation to the drug discovery/development and the therapeutic use of drugs. These includes: - animal and human pharmacological studies that focus on therapeutic response. pharmacodynamics, and toxicity related to plasma and tissue concentrations of drugs and their metabolites, - in vitro and in vivo drug absorption, distribution, metabolism, transport, and excretion studies that facilitate investigations related to the use of drugs in man - studies on membrane transport and enzymes, including their regulation and the impact of pharmacogenomics on drug absorption and disposition, - simulation and modeling in drug discovery and development - theoretical treatises - includes themed issues and reviews and exclude manuscripts on - bioavailability studies reporting only on simple PK parameters such as Cmax, tmax and t1/2 without mechanistic interpretation - analytical methods