Joint Disposition Properties and Comprehensive Pharmacokinetic Characterization of Antibody-Drug Conjugates

被引:2
作者
Liao, Kai H. [1 ,2 ]
Williams, Jason H. [1 ]
Palani, Santhosh [1 ,3 ]
Yin, Donghua [1 ]
Meng, Xu [1 ]
机构
[1] Pfizer Inc, 10555 Sci Ctr Dr,CB10-2220, San Diego, CA 92121 USA
[2] Arcus Biosci, Hayward, CA USA
[3] PFM Hlth Sci, San Francisco, CA USA
关键词
antibody-drug conjugate; pharmacometrics; drug-to-antibody ratio; linker stability; therapeutic index; CANCER-THERAPY; PHASE I/II; VEDOTIN; TROP-2; MODEL;
D O I
10.1208/s12248-022-00717-x
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Antibody-drug conjugates (ADCs) comprise 3 distinct parts: a specific antibody carrier (mAb), a linker, and a cytotoxic payload. Typical pharmacokinetic (PK) characterization of ADCs remains fragmented using separate noncompartmental analyses (NCA) of individual analytes, offering little insight into the dynamic relationships among the ADC components, and the safety and efficacy implications. As a result, it is exceedingly difficult to compare ADCs in terms of favorable PK characteristics. Therefore, there is a need for characterizing ADCs using the joint disposition properties critical for understanding the fate of an ADC complex and clinical implications. In this communication, we describe 3 joint disposition metrics (JDMs) for integrated NCA of ADCs based on a combination of common analytes of ADC, payload, conjugated payload, and total mAb. These JDMs were derived, each in a simple form of a ratio between appropriate PK parameters of two analytes, from the presumed drug delivery scheme behind typical ADC designs, in terms of (1) linker stability, (2) therapeutic exposure ratio, and (3) effective drug-toantibody ratio in vivo. The validity of the JDM-based PK characterization was examined against model-based analyses via their applications to 3 clinical candidates: PF-06650808, PF-06647020, and PF-06664178. For instance, the linker stability estimates for PF-06650808, PF-06647020, and PF-06664178 were 0.31, 0.14, and 0.096, respectively, from the JDM-based analyses vs. 0.23, 0.11, and 0.086 by the model-based approach. Additionally, the JDMs were estimated for a number of FDA-approved or otherwise well-documented ADCs, showing their utilities in comparing ADCs in terms of favorable PK characteristics.
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页数:12
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