The epidemiology of inhibitors in haemophilia A: a systematic review

Wight, Jeremy; Paisley, Suzy

doi:10.1046/j.1365-2516.2003.00780.x

Cited by 545 publications

(568 citation statements)

References 54 publications

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“…In a cohort of 316 subjects, Gouw et al found that there was no association between the type of product used and inhibitor development. 32 In addition, since the rate of nontransient inhibitor development in prospective trials of new recombinant products was similar to studies using plasmaderived products 33,34 ; and inhibitor formation is rare in previously treated patients who are switched to recombinant products 33,35,36 ; we believe the overall weight of the data suggests that there is no association between the type of fVIII product and inhibitor formation. Thus, we do not consider the risk of inhibitor formation when selecting a fVIII product to use for an individual patient.…”

Section: Treatment-related Risk Factorsmentioning

confidence: 62%

How we treat a hemophilia A patient with a factor VIII inhibitor

Kempton

White

2009

Blood

146

142

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The most significant complication of treatment in patients with hemophilia A is the development of alloantibodies that inhibit factor VIII activity. In the presence of inhibitory antibodies, replacement of the missing clotting factor by infusion of factor VIII becomes less effective. Once replacement therapy is ineffective, acute management of bleeding requires agents that bypass factor VIII activity. Long-term management consists of eradicating the inhibitor through immune tolerance. Despite success in the treatment of acute bleeding and inhibitor eradication, there remains an inability to predict or prevent inhibitor formation. Ideally, prediction and ultimately prevention will come with an improved understanding of how patientspecific and treatment-related factors work together to influence anti-factor VIII antibody production. (Blood. 2009;113: 11-17)

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Section: Treatment-related Risk Factorsmentioning

confidence: 62%

How we treat a hemophilia A patient with a factor VIII inhibitor

Kempton

White

2009

Blood

146

142

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“…Two systematic reviews published in 2003 showed a significantly lower incidence of inhibitor development with the use of single pdFVIII product over a single rFVIII product; these reviews are summarized in Table 3. 15,16 However, after adjusting for study design, study period, testing frequency, and median follow-up, these data lost statistical significance in the second larger review. 16 The above data are largely retrospective, and a multivariate analysis of the studies in the second review showed an overestimation of inhibitor development in the retrospective studies.…”

Section: Prophylaxismentioning

confidence: 97%

Current Controversies in the Formation and Treatment of Alloantibodies to Factor VIII in Congenital Hemophilia A

Kruse‐Jarres

2011

Hematology

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A is a rare bleeding disorder treated with numerous factor VIII (FVIII)-containing replacement concentrates. This treatment approach has led to the formation of alloantibodies that neutralize the FVIII activity (inhibitors) conveyed by these commercially available concentrates in ϳ 25% of patients with severe hemophilia A (FVIII activity Ͻ 1% of normal). This phenomenon significantly complicates the treatment of these patients and compromises the effectiveness and efficiency of these products to reverse or prevent bleeding complications. Studying the population with alloantibody inhibitors is imperative but difficult due to the overall small number of individuals affected and the heterogeneity within this limited group. Furthermore, few randomized clinical trials have been conducted to answer pertinent questions so many controversies persist. This article focuses on the conflicting data on the variables associated with alloantibody FVIII inhibitor development with a particular emphasis on age and intensity of first treatment, the role of primary prophylaxis regimens in modulating this phenomenon, and the degree of purity of FVIII product as a potential contributing risk factor. The optimal dosing regimen and type of FVIII replacement product that should be used to achieve the highest success rate in immune tolerance induction (ITI) protocols are also discussed, as well as whether the addition of immunomodulatory agents, especially rituximab, to ITI regimens enhances the durability of ITI and the eradication of alloantibody FVIII inhibitors.

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“…The development of antibodies that inhibit or neutralize factor VIII (FVIII) replacement therapy occurs in as many as 20% to 30% of patients with severe hemophilia A and represents one of the most serious complications of hemophilia [1][2][3]. Inhibitors typically develop in early childhood, within the first 10-20 exposures to FVIII concentrates [2].…”

Section: Introductionmentioning

confidence: 99%

Prevention of bleeds in hemophilia patients with inhibitors: Emerging data and clinical direction

Leissinger

2004

American J Hematol

101

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In patients with hemophilia, the development of high-responding inhibitors to factor VIII prevents adequate replacement therapy and results in increased risk of serious bleeding episodes, poor control of joint bleeding, and progressive, debilitating joint disease. Immune tolerance therapy can eradicate inhibitors, but it is not uniformly successful. Emerging data suggest that prophylaxis using activated prothrombin complex concentrates may be effective and safe in reducing the incidence of joint bleeding during immune tolerance therapy and for patients in whom immune tolerance induction fails. However, only controlled clinical trials will ultimately demonstrate whether prophylaxis can prevent joint bleeding and damage, and improve quality of life in patients with inhibitors. Am.

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The epidemiology of inhibitors in haemophilia A: a systematic review

Cited by 545 publications

References 54 publications

How we treat a hemophilia A patient with a factor VIII inhibitor

How we treat a hemophilia A patient with a factor VIII inhibitor

Current Controversies in the Formation and Treatment of Alloantibodies to Factor VIII in Congenital Hemophilia A

Prevention of bleeds in hemophilia patients with inhibitors: Emerging data and clinical direction

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