Informing pregnancy dose via target-mediated drug disposition modeling and simulations for a recombinant human monoclonal antibody

IF 3.1 3区 医学 Q2 PHARMACOLOGY & PHARMACY
Courtney Moc Willeford, Krithika Shetty, Douglas Sheridan, Frank Engler
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引用次数: 0

Abstract

RLYB212 is a human monoclonal anti-human platelet antigen (HPA)-1a immunoglobulin gamma 1 in clinical development as a subcutaneous injection for the prevention of maternal alloimmunization to fetal HPA-1a leading to fetal and neonatal alloimmune thrombocytopenia (FNAIT). This analysis developed a target-mediated drug disposition (TMDD) model to simultaneously characterize RLYB212 pharmacokinetics (PK) and HPA-1a-positive platelet dynamics in HPA-1b/b (HPA-1a-negative) volunteers. The model was then used to perform simulations to inform a dosing regimen in a phase II clinical study in pregnant women, where simulations accounted for physiological changes throughout pregnancy. Allometric scaling (0.75) for clearance and intercompartment transfer rate and volume (1) was included in the base model to account for variations in body weight. A 0.06 mg RLYB212 dose with a loading dose of 0.12 mg was identified as the optimal dosing regimen of RLYB212, which maintained exposures below the target upper boundary of ~10 ng/mL throughout pregnancy. This work presents an application of the TMDD model that advances the quantitative clinical pharmacology toolkit to understand monoclonal antibody PK in pregnancy.

通过对重组人单克隆抗体进行靶向药物处置建模和模拟,为妊娠剂量提供依据。
RLYB212 是一种人单克隆抗人血小板抗原 (HPA)-1a 免疫球蛋白 gamma 1,目前正作为皮下注射药物进行临床开发,以预防母体对胎儿 HPA-1a 的同种免疫导致胎儿和新生儿同种免疫血小板减少症 (FNAIT)。这项分析建立了一个靶向介导药物处置(TMDD)模型,以同时描述 RLYB212 在 HPA-1b/b (HPA-1a 阴性)志愿者体内的药代动力学(PK)和 HPA-1a 阳性血小板动力学。然后利用该模型进行模拟,为孕妇 II 期临床研究中的给药方案提供依据,模拟中考虑了整个孕期的生理变化。在基础模型中加入了清除率、室间转移率和容积(1)的异比例缩放(0.75),以考虑体重的变化。0.06 毫克的 RLYB212 剂量和 0.12 毫克的负荷剂量被确定为 RLYB212 的最佳给药方案,可在整个孕期将暴露量维持在目标上限(约 10 纳克/毫升)以下。这项工作展示了 TMDD 模型的应用,它推进了定量临床药理工具包的发展,有助于了解妊娠期单克隆抗体的 PK。
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
CiteScore
5.00
自引率
11.40%
发文量
146
审稿时长
8 weeks
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