Advances in Treatment for Haemophilia
Abstract
Traditional replacement therapy for haemophilia is limited by development of inhibitors, parenteral administration and short half-life of the protein. A number of new therapies are in development and reaching the clinic which can address all these problems. Firstly, modifications have been made to Factor VIII (FVIII) and Factor IX (FIX) which prolong their half-life without impairing function. The prolongation of approximately 1.5 times control for Factor VIII is relatively modest but for Factor IX it is 35-fold which allows prophylactic injections to be given every 7-14 days. A step further is the development of a bispecific antibody which mimics
the cofactor function of FVIII by binding to both Factor IXa and Factor X. A completely novel approach is to remedy the procoagulant deficiency in haemophilia by balancing it with a corresponding reduction in anticoagulant activity. All three anticoagulant pathways (TFPI, Protein C-Protein S and antithrombin) have been identified as targets for this 'rebalancing' approach to therapy, which has been successful in preliminary trials. These new therapies have the advantage that they will not stimulate anti-FVIII or FIX antibodies and will be able to work effectively even if they are present. Moreover, they can be given by subcutaneous injection and have much longer half-lives that FVIII or FIX. However, they may be difficult to monitor and to combine safely with other treatments. Finally, the success of early trials with gene therapy offer the prospect of freeing patients from injections entirely and elevating their FVIII or IX levels into the range sufficient to secure normal haemostasis.
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