40K glyco PEG ylated, recombinant FVII a: 3‐month, double‐blind, randomized trial of safety, pharmacokinetics and preliminary efficacy in hemophilia patients with inhibitors

Summary Background A 40K glyco PEG ylated, recombinant activated f actor VII ( rFVII a) bypassing agent (N7‐ GP ) with a prolonged half‐life (15 h) compared with rFVII a was developed as a potential candidate for bleed‐preventive regimens in patients with hemophilia and inhibitors. Objectives To evaluate the safety, pharmacokinetics and preliminary efficacy of multiple doses of N7‐ GP in congenital hemophilia A and B patients with high‐titer inhibitors. Patients/Methods In this global, prospective, randomized, double‐blinded, phase 2 trial, 25, 100 or 200 μg kg −1  N7‐ GP was administered intravenously once every second day during a 3‐month, bleed‐preventive regimen and compared with a preceding 3‐month observation period with on‐demand treatment of bleeds with rFVII a. The primary endpoint was adverse events; secondary endpoints were evaluation of immunogenicity, pharmacokinetics and efficacy. Results and Conclusions Overall, 23 patients were randomized and dosed ( n  =   8/7/8 for 25/100/200 μg kg −1 ). N7‐ GP was well tolerated, with a low frequency of adverse events. No serious adverse events, immunogenic or thromboembolic events related to N7‐ GP were reported. The pharmacokinetic properties of N7‐ GP were similar to those reported in phase 1. The annualized bleeding rate ( ABR ) decreased in the treatment period vs. the observation period at all N7‐ GP dose levels. However, a dose‐response relationship in the reduction could not be established in the N7‐ GP dose range evaluated. The ABR was also reduced at two dose levels during the last part of the observation period, and increased notably in the follow‐up period irrespective of previous N7‐ GP dose. The trial was registered at ClinicalTrials.gov (Registration Number: NCT 00951405).