Literature DB >> 26047352

Structure-guided residence time optimization of a dabigatran reversal agent.

Felix Schiele1, Joanne van Ryn, Tobias Litzenburger, Michael Ritter, Daniel Seeliger, Herbert Nar.   

Abstract

Novel oral anticoagulants are effective and safe alternatives to vitamin-K antagonists for anticoagulation therapy. However, anticoagulation therapy in general is associated with an elevated risk of bleeding. Idarucizumab is a reversal agent for the direct thrombin inhibitor, dabigatran etexilate (Pradaxa®) and is currently in Phase 3 studies. Here, we report data on the antibody fragment aDabi-Fab2, a putative backup molecule for idarucizumab. Although aDabi-Fab2 completely reversed effects of dabigatran in a rat model in vivo, we observed significantly reduced duration of action compared to idarucizumab. Rational protein engineering, based on the X-ray structure of aDabi-Fab2, led to the identification of mutant Y103W. The mutant had optimized shape complementarity to dabigatran while maintaining an energetically favored hydrogen bond. It displayed increased affinity for dabigatran, mainly driven by a slower off-rate. Interestingly, the increased residence time translated into longer duration of action in vivo. It was thus possible to further enhance the efficacy of aDabi-Fab2 based on rational design, giving it the potential to serve as a back-up candidate for idarucizumab.

Entities:  

Keywords:  Pradaxa; antidote; idarucizumab; rational protein design; residence time; thrombin

Mesh:

Substances:

Year:  2015        PMID: 26047352      PMCID: PMC4622598          DOI: 10.1080/19420862.2015.1057364

Source DB:  PubMed          Journal:  MAbs        ISSN: 1942-0862            Impact factor:   5.857


  42 in total

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