AI Article Synopsis
- The development of alloantibodies against factor VIII is a major complication in treating congenital hemophilia A, affecting patient outcomes.
- During a study from 1993 to 2006, data was collected on patients' inhibitor tests and factor infusions, showing that 12% tested positive for inhibitors at least twice.
- Most patients with low inhibitor levels (< 5 BU/ml) achieved a sustained negative status, suggesting that immune tolerance induction may not be necessary for those with lower inhibitor titres.
- Further research is needed to identify factors influencing sustained negative status in regions lacking ITI treatment options.
Article Abstract
The development of alloantibodies that inhibit or neutralise the function of factor VIII is considered the most serious complication of the treatment of congenital haemophilia A. In order to describe their course without immune tolerance induction (ITI), we documented data on all performed inhibitor tests with dates as well as on clotting factor infusions of all consecutive patients who were treated in our centre between 1993 and 2006. Patients were tested every 7.1 months (95% confidence interval [CI], 6.6-7.8). A 'sustained negative inhibitor status' was defined as consistent non-positive inhibitor measurements for two years or longer. A total of 60/486 (12%) patients tested had a positive inhibitor titre in two or more occasions. Most of the patients (56%) with a maximum inhibitor titre of < 5 Bethesda unit (BU)/ml (named "low titre inhibitor") developed a sustained negative inhibitor status. Among patients with high (5-9.9 BU/ml) and very high (≥ 10 BU/ml) inhibitor titres, the proportions were 50% and 3%, respectively. Our findings suggest that ITI might not be needed for all patients with non-transient inhibitors, especially when their maximum inhibitor titre is below 10 BU/ml. Further studies in countries where ITI is not available are needed to examine predictors of the natural sustained negative inhibitor status.
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| http://dx.doi.org/10.1160/TH10-04-0231 | DOI Listing |
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