A Semimechanistic Ocular Pharmacokinetic Model for ADVM-022 Gene Therapy Describing the Dose-Exposure Relationship in Monkeys and the Scaling to Human.

IF 4.5 2区医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL

Molecular Pharmaceutics Pub Date : 2025-07-21 DOI:10.1021/acs.molpharmaceut.5c00155

Florian Hugi, Jannik Vollmer, Lionel Renaud, Matthias Machacek

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引用次数: 0

Abstract

Gene therapies are emerging as a new treatment modality. Due to their novelty, general pharmacological properties have yet to be established. For example, the translation from animal models to humans for first-in-human dose selection and the dose-exposure relationship remain poorly characterized. A mechanistic and quantitative framework would improve preclinical program design, enable more robust first-in-human dose predictions, and support more rigorous dose adjustments during clinical development. This study establishes a semimechanistic mathematical model for aflibercept expression and pharmacokinetics (PK) following intravitreal (IVT) ADVM-022 administration in monkeys and humans, drawing on the preclinical and clinical data presently available. ADVM-022 is an AAV2.7m8-based viral vector that delivers the gene encoding aflibercept, an antivascular endothelial growth factor (VEGF) fusion protein. It was developed as a gene therapy for treating wet age-related macular degeneration (wAMD) and is administered through a single IVT injection. The proposed model incorporates established ocular PK for intravitreally administered proteins, along with an expression component that links AAV dose to aflibercept production. Based on pooled PK data from monkey studies, the model suggests that transduction occurs not only in the retina but also in other ocular tissues bordering the vitreous, contributing to the observed intraocular aflibercept levels. Increasing doses within the lower range of preclinical studies (3 × 10¹⁰-2 × 10¹³ vg/eye) lead to increased transduction and expression, plateauing at upper limits of approximately 12.7 μg/day·cm³ for the retina, and 0.785 μg/day for extra-retinal tissues at higher doses. Assuming similar transduction efficiency between humans and monkeys, with adjustments for anatomical differences, the model provided predictions of ocular aflibercept concentrations that aligned with observations from the two dose groups in the phase 1 OPTIC clinical trial, supporting the utility of this approach.

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ADVM-022基因治疗的半机械眼药代动力学模型及其在猴子体内剂量-暴露关系的研究。

基因治疗正在成为一种新的治疗方式。由于它们的新颖性，一般的药理学性质尚未确定。例如，从动物模型到人类的首次人体剂量选择的转换和剂量-暴露关系的特征仍然很差。机制和定量框架将改进临床前项目设计，实现更可靠的首次人体剂量预测，并在临床开发期间支持更严格的剂量调整。本研究利用目前可用的临床前和临床数据，建立了猴和人玻璃体内给药ADVM-022后aflibercept表达和药代动力学（PK）的半机械数学模型。ADVM-022是一种基于aav2.7 m8的病毒载体，可传递编码afliberept的基因，afliberept是一种抗血管内皮生长因子（VEGF）融合蛋白。它是一种用于治疗湿性年龄相关性黄斑变性（wAMD）的基因疗法，通过单次IVT注射进行治疗。所提出的模型结合了玻璃体内给药蛋白的已建立的眼部PK，以及将AAV剂量与阿伯西普产生联系起来的表达成分。基于猴子研究的PK数据，该模型表明，转导不仅发生在视网膜上，也发生在玻璃体周围的其他眼部组织中，这有助于观察到眼内afliberept水平。在临床前研究的较低范围内（3 × 1010-2 × 1013 vg/眼）增加剂量导致转导和表达增加，在视网膜的上限约为12.7 μg/天·cm3，在视网膜外组织的较高剂量为0.785 μg/天。假设人类和猴子之间的转导效率相似，并对解剖差异进行了调整，该模型提供了与两个剂量组在1期OPTIC临床试验中的观察结果一致的眼部afliberceept浓度预测，支持了该方法的实用性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Molecular Pharmaceutics 医学-药学

CiteScore

8.00

自引率

6.10%

发文量

391

审稿时长

2 months

期刊介绍： Molecular Pharmaceutics publishes the results of original research that contributes significantly to the molecular mechanistic understanding of drug delivery and drug delivery systems. The journal encourages contributions describing research at the interface of drug discovery and drug development. Scientific areas within the scope of the journal include physical and pharmaceutical chemistry, biochemistry and biophysics, molecular and cellular biology, and polymer and materials science as they relate to drug and drug delivery system efficacy. Mechanistic Drug Delivery and Drug Targeting research on modulating activity and efficacy of a drug or drug product is within the scope of Molecular Pharmaceutics. Theoretical and experimental peer-reviewed research articles, communications, reviews, and perspectives are welcomed.