Authors’ Reply to Kamel et al.: “Effect of Age and Renal Function on Idarucizumab Pharmacokinetics and Idarucizumab-Mediated Reversal of Dabigatran Anticoagulant Activity in a Randomized, Double-Blind, Crossover Phase Ib Study”

We thank Dr. Kamel and colleagues for their valuable comments [1] and would like to provide the following response to the questions raised. The unbound dabigatran concentration reflects the level of active dabigatran in the blood. Administration of idarucizumab 5 g to volunteers of various age groups and with different degrees of renal impairment reduced unbound dabigatran concentrations to below the lower limit of quantitation (LLOQ) (1 ng/mL). Approximately 12–16 h post-idarucizumab administration, an increase in the concentrations of unbound dabigatran above the LLOQ was noted. Importantly, the underlying detection methodology is highly sensitive and, over the entire observation period, levels did not increase above the threshold for pharmacological activity. Consequently, coagulation time measurements also did not increase above their respective upper limits of normal, as illustrated for activated partial thromboplastin time in Table 1. A 5 g dose of idarucizumab completely neutralizes dabigatran anticoagulation in almost all patients, as demonstrated by coagulation time measurements in dabigatran-treated patients receiving idarucizumab as emergency treatment [2]. Coagulation time measurements are frequently applied as routine measures in clinical emergency settings, and the results can provide important information supporting rational treatment decisions. In REVERSE AD (REVERSal Effects of idarucizumab in patients on Active Dabigatran), patients’ coagulation times were determined up to 24 h after idarucizumab administration [2]. In this timeframe most clinical emergencies are expected to resolve. A re-occurrence of dabigatran anticoagulation was noted in some patients, mostly 12–24 h after idarucizumab administration [2]. Importantly, almost none of these patients were bleeding, suggesting that for these patients the re-elevation was not clinically relevant. However, as pointed out by Dr. Kamel and colleagues [1], there are certain clinical situations in which a re-occurrence of the anticoagulant effect of dabigatran might be harmful. Consequently, a second dose of idarucizumab was allowed in the RE-VERSE AD clinical trial; the respective data will be available in the final publication when the trial is complete. Consideration of an additional dose is also proposed in the idarucizumab label. The criteria for the additional dose focus on both the clinical condition of the patient as well as the coagulation status: