Pathogenic immune response to therapeutic factor VIII: exacerbated response or failed induction of tolerance?

Pathogenic immune response to therapeutic factor VIII: exacerbated response or failed induction of tolerance?

Therapeutic factor VIII is highly immunogenic. Despite intensive research in the last decades, the reasons why 5-30% of patients with hemophilia A (of all severities) develop inhibitory anti-factor VIII antibodies (inhibitors) following replacement therapy remain an enigma. Under physiological condi...

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Veröffentlicht in:Haematologica (Roma) 2019-02, Vol.104 (2), p.236-244
Hauptverfasser: Varthaman, Aditi, Lacroix-Desmazes, Sébastien
Format: Artikel
Sprache:eng
Schlagworte:
Blood Coagulation Factor Inhibitors - immunology
Factor VIII - administration & dosage
Factor VIII - immunology
Factor VIII - therapeutic use
Hemophilia A - blood
Hemophilia A - complications
Hemophilia A - drug therapy
Hemophilia A - immunology
Hemorrhage - etiology
Humans
Immune System - immunology
Immune System - metabolism
Immune Tolerance
Immunology
Inflammation - complications
Inflammation - metabolism
Isoantibodies - immunology
Life Sciences
Review
T-Lymphocyte Subsets - immunology
T-Lymphocyte Subsets - metabolism
Treatment Failure
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Zusammenfassung:Therapeutic factor VIII is highly immunogenic. Despite intensive research in the last decades, the reasons why 5-30% of patients with hemophilia A (of all severities) develop inhibitory anti-factor VIII antibodies (inhibitors) following replacement therapy remain an enigma. Under physiological conditions, endogenous factor VIII is recognized by the immune system. Likewise, numerous observations indicate that, in hemophilia A patients without inhibitors, exogenous therapeutic factor VIII is immunologically assessed and tolerated. A large part of the research on the immunogenicity of therapeutic factor VIII is attempting to identify the 'danger signals' that act as adjuvants to the deleterious anti-factor VIII immune responses. However, several of the inflammatory assaults concomitant to factor VIII administration initially hypothesized as potential sources of danger signals (e.g., bleeding, infection, and vaccination) have been disproved to be such signals. Conversely, recent evidence suggests that cells from inhibitor-negative patients are able to activate anti-inflammatory and tolerogenic mechanisms required to suppress deleterious immune responses, while cells from inhibitor-positive patients are not. Based on the available observations, we propose a model in which all hemophilia A patients develop anti-factor VIII immune responses during replacement therapy irrespective of associated danger signals. We further postulate that the onset of clinically relevant factor VIII inhibitors results from an inability to develop counteractive tolerogenic responses to exogenous factor VIII rather than from an exacerbated activation of the immune system at the time of factor VIII administration. A better understanding of the pathogenesis of neutralizing anti-factor VIII antibodies will have repercussions on the clinical management of patients and highlight new strategies to achieve active immune tolerance to therapeutic factor VIII.
ISSN:0390-6078
1592-8721
DOI:10.3324/haematol.2018.206383