A mechanistic pharmacokinetic model with drug and antidrug antibody interplay, and its application for assessing the impact of immunogenicity response on bioequivalence testing

Liao Kai H.; Udata Chandrasekhar; Yin Donghua; Sewell K. Lea; Kantaridis Constantino; Alvarez Daniel F.; Meng Xu

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A mechanistic pharmacokinetic model with drug and antidrug antibody interplay, and its application for assessing the impact of immunogenicity response on bioequivalence testing

机译：具有药物和抗皱抗体相互作用的机械药代理模型，及其评估免疫原性反应对生物等效测试的影响

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Aims Single-dose pharmacokinetic (PK) studies in healthy subjects have been the design of choice for bioequivalence determination for decades. This preference has been recently extended to PK similarity studies of proposed biosimilars. However, PK similarity studies can be complicated by the effect of immunogenicity response on drug disposition. The impact is exacerbated when there is an imbalance in host-specific immunological characteristics of subjects between the test and reference groups. Such complications remain poorly understood. The purpose of this communication is to show that the impact of immunogenicity response on PK similarity determination can be critical, using adalimumab as an example.

机译：目的几十年来，健康受试者单剂量药代动力学（PK）研究一直是生物等效性测定的首选设计。最近，这一偏好已扩展到拟用生物仿制药的PK相似性研究。然而，PK相似性研究可能因免疫原性反应对药物处置的影响而变得复杂。当试验组和对照组之间受试者的宿主特异性免疫学特征不平衡时，这种影响会加剧。人们对这种复杂情况仍知之甚少。本通讯的目的是以阿达木单抗为例，表明免疫原性反应对PK相似性测定的影响可能至关重要。

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来源
《British Journal of Clinical Pharmacology》 |2020年第11期|共10页
作者
Liao Kai H.; Udata Chandrasekhar; Yin Donghua; Sewell K. Lea; Kantaridis Constantino; Alvarez Daniel F.; Meng Xu;
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作者单位

Pfizer Inc 10777 Sci Ctr Dr San Diego CA 92121 USA;

Pfizer Inc 10777 Sci Ctr Dr San Diego CA 92121 USA;

Pfizer Inc 10777 Sci Ctr Dr San Diego CA 92121 USA;

Pfizer Inc Cambridge MA USA;

Pfizer Inc Brussels Belgium;

Pfizer Inc Collegeville PA USA;

Pfizer Inc 10777 Sci Ctr Dr San Diego CA 92121 USA;

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原文格式 PDF
正文语种 eng
中图分类药理学;
关键词
biosimilar; immunogenicity; pharmacokinetics;

机译：生物素质;免疫原性;药代动力学;

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A mechanistic pharmacokinetic model with drug and antidrug antibody interplay, and its application for assessing the impact of immunogenicity response on bioequivalence testing

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