Semorinemab Pharmacokinetics and The Effect on Plasma Total Tau Pharmacodynamics in Clinical Studies

IF 4.3 Q2 BUSINESS

The Journal of Prevention of Alzheimer's Disease Pub Date : 2024-07-17 DOI:10.14283/jpad.2024.146

Vidya Ramakrishnan, B. Bender, J. Langenhorst, M. O. Magnusson, M. Dolton, J. Shim, R. N. Fuji, C. Monteiro, E. Teng, N. Kassir, J. Jin

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Abstract

Background

Semorinemab is a monoclonal antibody that targets the N-terminal domain of the tau protein that is in clinical development for the treatment of Alzheimer’s disease.

Objectives

To perform model-based evaluations of the observed pharmacokinetics in serum and the total plasma tau target-engagement dynamics from clinical studies evaluating semorinemab.

Design

The observed semorinemab pharmacokinetics and plasma tau target engagement from phase 1 and 2 clinical studies were modeled using a non-linear mixed effect targetmediated drug disposition model. The model was simulated to understand target engagement at clinical dose levels.

Settings and Participants

The clinical studies testing semorinemab were evaluated in healthy volunteers, subjects with prodromal-to-mild Alzheimer’s disease, and subjects with mild-to-moderate Alzheimer’s disease. The data included a total of 8430 semorinemab serum concentrations and 4772 total tau protein plasma concentrations from 463 subjects treated with a range of single and multiple doses of semorinemab.

Measurements

Serum concentrations of semorinemab and the total plasma tau concentrations were measured after administration of a range of doses of semorinemab to subjects with Alzheimer’s disease. A sensitivity analysis was performed wherein key target-mediated drug disposition model parameters were estimated separately between healthy volunteers, subjects with prodromal-to-mild Alzheimer’s disease, and subjects with mild-to-moderate Alzheimer’s disease.

Results

Serum concentrations of semorinemab were consistent across studies and showed a dose-proportional increase across the evaluated dose range. The pharmacokinetic profile was comparable between healthy volunteers and subjects with Alzheimer’s disease. Total plasma tau concentrations increased in a dose-dependent non-linear manner upon semorinemab administration. The target-mediated drug disposition model adequately described the serum pharmacokinetics and protein dynamics with an estimated antibody-ligand binding strength, K_ss, of 42.7 nM. The estimated values of clearance and central volume of distribution were 0.109 L/day/70 kg and 2.95 L/70 kg, respectively, and were consistent with typical values for IgG mAbs. In the sensitivity analysis, K_ss (32 nM) and baseline tau protein (0.30 µM) were estimated to be lower for healthy volunteers compared to subjects with Alzheimer’s disease but were comparable between subjects with Alzheimer’s disease of different severities (K_ss: 52–57 nM, baseline tau: 0.44–0.47 µM). The models suggested that peripheral target engagement was over 90% at the clinical doses in each of the diagnostic subgroups.

Conclusion

Our target-mediated drug disposition model adequately described the serum pharmacokinetics and the peripheral non-linear increase with dose of the total tau. The model confirmed that these dose-response relationships were consistent across populations of healthy volunteers and subjects with different severities of Alzheimer’s disease.

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临床研究中塞莫瑞尼单抗的药代动力学及其对血浆总 Tau 药效学的影响

背景Semorinemab是一种靶向tau蛋白N端结构域的单克隆抗体，目前正处于治疗阿尔茨海默病的临床开发阶段。目的对评估semorinemab的临床研究中观察到的血清中药代动力学和总血浆tau靶向参与动态进行基于模型的评估。设置和参与者在健康志愿者、前驱期至轻度阿尔茨海默病患者以及轻度至中度阿尔茨海默病患者中评估了测试semorinemab的临床研究。这些数据包括463名受试者在服用一系列单剂量或多剂量的舍莫瑞单抗后，血清中舍莫瑞单抗的浓度和血浆中总tau蛋白的浓度，总计分别为8430和4772。进行了一项敏感性分析，分别估算了健康志愿者、前驱期至轻度阿尔茨海默氏症患者和轻度至中度阿尔茨海默氏症患者的关键靶向药物处置模型参数。结果在各项研究中，塞莫瑞单抗的血清浓度是一致的，并且在评估的剂量范围内呈现剂量比例增长。健康志愿者和阿尔茨海默病患者的药代动力学特征相当。服用semorinemab后，血浆tau总浓度呈剂量依赖性非线性增加。靶向介导的药物处置模型充分描述了血清药代动力学和蛋白质动力学，估计抗体与配体的结合强度（Kss）为42.7 nM。清除率和中心分布容积的估计值分别为 0.109 升/天/70 千克和 2.95 升/70 千克，与 IgG mAbs 的典型值一致。在敏感性分析中，健康志愿者的 Kss（32 nM）和基线 tau 蛋白（0.30 µM）估计值低于阿尔茨海默氏症患者，但与不同严重程度的阿尔茨海默氏症患者相当（Kss：52-57 nM，基线 tau：0.44-0.47 µM）。结论我们的靶向介导药物处置模型充分描述了总 tau 的血清药代动力学和外周非线性剂量增加。该模型证实，这些剂量-反应关系在健康志愿者和患有不同严重程度阿尔茨海默病的受试者群体中是一致的。

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

The Journal of Prevention of Alzheimer's Disease Medicine-Psychiatry and Mental Health

CiteScore

9.20

自引率

0.00%

发文量

期刊介绍： The JPAD Journal of Prevention of Alzheimer’Disease will publish reviews, original research articles and short reports to improve our knowledge in the field of Alzheimer prevention including: neurosciences, biomarkers, imaging, epidemiology, public health, physical cognitive exercise, nutrition, risk and protective factors, drug development, trials design, and heath economic outcomes.JPAD will publish also the meeting abstracts from Clinical Trial on Alzheimer Disease (CTAD) and will be distributed both in paper and online version worldwide.We hope that JPAD with your contribution will play a role in the development of Alzheimer prevention.