| Literature DB >> 29571739 |
Chuenlei Parng1, Pratap Singh2, Debra D Pittman3, Katherine Wright2, Beth Leary2, Sunita Patel-Hett3, Swapnil Rakhe3, James Stejskal4, Marjorie Peraza4, Dawn Dufield2, John E Murphy3, Rob Webster2.
Abstract
Tissue factor pathway inhibitor (TFPI) exhibits multiple isoforms, which are known to present in multiple locations such as plasma, endothelium, and platelets. TFPI is an endogenous negative modulator of the coagulation pathway, and therefore, neutralization of TFPI function can potentially increase coagulation activity. A human monoclonal antibody, PF-06741086, which interacts with all isoforms of TFPI is currently being tested in clinic for treating hemophilia patients with and without inhibitors. To support clinical development of PF-06741086, pharmacokinetics (PK) and pharmacodynamics of PF-06741086 were characterized in monkeys. In addition, a mechanistic model approach was used to estimate PK parameters in monkeys and simulate PK profiles in human. The results show that PF-06741086 exhibited target-mediated drug disposition and had specific effects on various hemostatic markers including diluted prothrombin time, thrombin generation, and thrombin-antithrombin complex in monkeys after administration. The model-predicted and observed human exposures were compared retrospectively, and the result indicates that the exposure prediction was reasonable within less than 2-fold deviation. This study demonstrated in vivo efficacy of PF-06741086 in monkeys and the utility of a rational mechanistic approach to describe PK for a monoclonal antibody with complex target binding.Entities:
Keywords: TFPI; TMDD; human dose projection; mechanistic modeling; monoclonal antibody; non-linear pharmacokinetics; pharmacodynamics
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Year: 2018 PMID: 29571739 DOI: 10.1016/j.xphs.2018.03.010
Source DB: PubMed Journal: J Pharm Sci ISSN: 0022-3549 Impact factor: 3.534