Development of inhibitory antibodies to therapeutic factor VIII in severe hemophilia A is associated with microsatellite polymorphisms in the HMOX1 promoter

Repessé, Yohann; Peyron, Ivan; Dimitrov, Jordan D.; Dasgupta, Suryasarathi; Moshai, Elika Farrokhi; Costa, Cathérine; Borel‐Derlon, Annie; Guillet, Benoît; d’Oiron, Roseline; Aouba, Achille; Rothschild, Chantal; Oldenburg, Johannes; Pavlova, Anna; Kaveri, Srini V.; Lacroix‐Desmazes, Sébastien

doi:10.3324/haematol.2013.084665

Cited by 36 publications

(37 citation statements)

References 43 publications

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“…Up to 30% of hemophilia A patients develop antibodies against recombinant human Factor VIII (Ehrenforth et al, 1992;Repesse et al, 2013). We used mice deficient in Factor VIII (Bi et al, 1995;Delignat et al, 2012;Qian et al, 1999) to assess the effect of complement depletion with hCVF protein HC3-1496 on the production on a Human PNH cells were incubated in the presence of rH19-20 with normal human serum or human serum complement-depleted with hCVF or CVF.…”

Section: Hemophilia Amentioning

confidence: 99%

Humanized cobra venom factor: Structure, activity, and therapeutic efficacy in preclinical disease models

Vogel

Finnegan²,

Fritzinger

2014

Molecular Immunology

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Section: Hemophilia Amentioning

confidence: 99%

Humanized cobra venom factor: Structure, activity, and therapeutic efficacy in preclinical disease models

Vogel

Finnegan²,

Fritzinger

2014

Molecular Immunology

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“…A useful approach, therefore, is to prevent inhibitor development in the first phase of the immune response. Some potential strategies for inhibitor prevention may include : ‘Deimmunization’ of FVIII whereby amino acid residues that serve as contact sites are eliminated. Modification of FVIII domains (i.e. C1) to prevent its uptake by dendritic cells, e.g.…”

Section: Fviii‐specific B‐cell‐mediated Immune Responsementioning

confidence: 99%

New predictive approaches for ITI treatment

et al. 2014

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Summary Immune tolerance induction (ITI) therapy in patients with haemophilia A and inhibitors constitutes a huge burden for affected patients and families and poses a large economic burden for a chronic disease. Concerted research efforts are attempting to optimize the therapeutic approach to the prevention and eradication of inhibitors. The Italian ITI Registry has provided data on 110 patients who completed ITI therapy as at July 2013. Analysis of independent predictors of success showed that, together with previously recognized factors – namely inhibitor titre prior to ITI, historical peak titre and peak titre on ITI – the type of causative FVIII gene mutation also contributes to the identification of patients with good prognosis and may be useful to optimize candidate selection and treatment regimens. Numerous studies have demonstrated that inhibitor reactivity against different FVIII products varies and is lower against concentrates containing von Willebrand factor (VWF). An Italian study compared inhibitor titres against a panel of FVIII concentrates in vitro and correlated titres with the capacity to inhibit maximum thrombin generation as measured by the thrombin generation assay (TGA). Observations led to the design of the PredictTGA study which aims to correlate TGA results with epitope specificity, inhibitor reactivity against different FVIII concentrates and clinical data in inhibitor patients receiving FVIII in the context of ITI or as prophylactic/on demand treatment. At the immunological level, it is known that T cells drive inhibitor development and that B cells secrete FVIII‐specific antibodies. As understanding increases about the immunological response in ITI, it is becoming apparent that modulation of T‐cell‐ and B‐cell‐mediated responses offers a range of potential new and specific approaches to prevent and eliminate inhibitors as well as individualize ITI therapy.

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“…22 Thus, the recent report of associations between inhibitor development and polymorphisms in the HMOX-1 gene is of interest and requires further follow-up. 23 Tregs have also been implicated in the process of inducing tolerance in patients with an established memory using immune tolerance induction (ITI) therapy. Here, frequent exposure to the deficient factor in the absence of systemic inflammation may induce Tregs with a subsequent lack of T-helper cells, preventing B-cell differentiation and promoting tolerance through B-cell anergy and/or deletion.…”

mentioning

confidence: 99%

FVIII inhibitors: pathogenesis and avoidance

Astermark

2015

Blood

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The pathogenesis of inhibitory antibodies has been the focus of major scientific interest over the last decades, and several studies on underlying immune mechanisms and risk factors for formation of these antibodies have been performed with the aim of improving the ability to both predict and prevent their appearance. It seems clear that the decisive factors for the immune response to the deficient factor are multiple and involve components of both a constitutional and therapy-related nature. A scientific concern and obstacle for research in the area of hemophilia is the relatively small cohorts available for studies and the resulting risk of confounded and biased results. Careful interpretation of data is recommended to avoid treatment decisions based on a weak scientific platform. This review will summarize current concepts of the underlying immunological mechanisms and risk factors for development of inhibitory antibodies in patients with hemophilia A and discuss how these findings may be interpreted and influence our clinical management of patients. (Blood. 2015;125(13):2045-2051 IntroductionUnderstanding of the pathophysiological mechanisms leading to the development of inhibitory anti-factor (F)VIII antibodies in patients with hemophilia A has improved considerably over the last 2 decades. It is clear that the process is multifactorial and involves cells, cytokines, and other immune regulatory molecules, the level and action of which are both genetically and nongenetically defined. Despite improvements in understanding, we remain unable to fully predict the immune response to the deficient factor and inhibitor risk at the onset of replacement therapy. There are several ongoing efforts aiming to achieve more accurate methods for prediction and others to develop nonimmunogenic hemostatic options, but these remain opportunities for the future. Findings continue to emerge regarding risk factors and potential immune mechanisms of significance for the outcome, but until new results have been sufficiently confirmed through replication and the mechanisms of action in humans better defined, the chances of withholding a beneficial treatment or administering one associated with an adverse outcome are increased. Efficacy and safety should be the guiding principles for all treaters in the environment of cost constraints in which they act. This review will summarize current data-based findings and interpretations of how and why inhibitory antibodies develop in patients with hemophilia A and explore how the findings may or may not influence our daily practice. Immune response to FVIIIThe initiation of an immune response and formation of high-affinity polyclonal antibodies toward FVIII requires endocytosis of the infused molecule by antigen presenting cells (APCs), eg, dendritic cells, macrophages, and/or B cells, processing intracellularly in the endosomes, and presentation of antigen-derived peptides via the HLA class II molecules on the cell surface to the CD4 1 T cells. In previously untreated patients, ie, patients...

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Development of inhibitory antibodies to therapeutic factor VIII in severe hemophilia A is associated with microsatellite polymorphisms in the HMOX1 promoter

Cited by 36 publications

References 43 publications

Humanized cobra venom factor: Structure, activity, and therapeutic efficacy in preclinical disease models

Humanized cobra venom factor: Structure, activity, and therapeutic efficacy in preclinical disease models

New predictive approaches for ITI treatment

FVIII inhibitors: pathogenesis and avoidance

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