Inhibitor Development in Previously Untreated Patients with Severe Hemophilia a Treated with Nuwiq®, a New Generation Recombinant FVIII of Human Origin

Liesner, Raina; Abashidze, Marina; Алейникова, О. В.; Altisent, Carmen; Belletrutti, Mark; Borel‐Derlon, Annie; Carção, Manuel; Chambost, Hérvè; Chan, Anthony; Dubey, Leonid; Ducore, Jonathan M.; Abubacker, Fouzia N.; Gattens, Michael; Gruel, Yves; Kavardakova, N.; Khorassani, Mohamed El; Klukowska, Anna; Königs, Christoph; Lambert, Thierry; Lohade, Sunil; Sigaud, Marianne; Ţurea, Valentin; Wu, John; Vdovin, Vladimír

doi:10.1182/blood.v128.22.327.327

Cited by 4 publications

(6 citation statements)

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“…The cumulative incidence of all inhibitors was 20.8% (95% CI 10.68–30.95) and of high-titer inhibitor was 12.8% (95% CI 4.49–21.25). 36 Whether these preliminary results will hold and can be compared with other clinical trial results remain to be seen. Final study results are expected in 2018.…”

Section: Standard Half-life Fviii Productsmentioning

confidence: 98%

Current and emerging factor VIII replacement products for hemophilia A

Cafuir

Kempton

2017

Therapeutic Advances in Hematology

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Hemophilia A is a congenital X-linked bleeding disorder caused by coagulation factor VIII (FVIII) deficiency. Routine infusion of factor replacement products is the current standard of care; however, the development of alloantibodies against FVIII remains a challenge. The treatment of hemophilia has undergone major advances over the past century to improve safety, effectiveness, manufacturing, and convenience of factor products. Major recent advances in the treatment of hemophilia A include the emergence of extended half-life products, factor VIII orthologs, and gene therapy products. Extended half-life products were designed to decrease the frequency of infusions, but only modest half-life extension is achieved. Factor VIII orthologs featuring lower cross-reactivity with anti-FVIII antibodies may be less susceptible to inactivation by inhibitors. Meanwhile, gene therapy may potentially provide a cure for hemophilia A, thus abrogating the need for protein-based factor replacement. This review aims to discuss current and emerging FVIII replacement products for hemophilia A.

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Section: Standard Half-life Fviii Productsmentioning

confidence: 98%

Current and emerging factor VIII replacement products for hemophilia A

Cafuir

Kempton

2017

Therapeutic Advances in Hematology

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“…199 Interim analysis of the immunogenicity of a new B-domain-modified product with an alternative linker with a partial non-FVIII sequence (Figure 1B; Nuwiq, Antihemophilic Factor [Recombinant]) designed to facilitate expression in human cell lines suggests this strategy may have a lower inhibitor risk than other FVIII variants expressed from non-human cell lines. 200 Likewise, there have been no reports to date of the development of new anti-FVIII antibodies against BAY 94-9027 (Jivi, antihemophilic factor [recombinant], PEGylated-aucl), which is a recently approved EHL FVIII product with the substitution K1804C (in the A3 domain) introduced to allow site-specific pegylation. 201,202 There have also been no reports of anti-FIX antibodies in the R16 subjects who have received FIX-Padua gene therapy (P.E.…”

Section: Protein-engineered Bypassing Agentsmentioning

confidence: 99%

Protein-Engineered Coagulation Factors for Hemophilia Gene Therapy

Samelson-Jones

Arruda

2019

Molecular Therapy - Methods & Clinical Development

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Hemophilia A (HA) and hemophilia B (HB) are X-linked bleeding disorders due to inheritable deficiencies in either coagulation factor VIII (FVIII) or factor IX (FIX), respectively. Recently, gene therapy clinical trials with adeno-associated virus (AAV) vectors and protein-engineered transgenes, B-domain deleted (BDD) FVIII and FIX-Padua, have reported near-phenotypic cures in subjects with HA and HB, respectively. Here, we review the biology and the clinical development of FVIII-BDD and FIX-Padua as transgenes. We also examine alternative bioengineering strategies for FVIII and FIX, as well as the immunological challenges of these approaches. Other engineered proteins and their potential use in gene therapy for hemophilia with inhibitors are also discussed. Continued advancement of gene therapy for HA and HB using protein-engineered transgenes has the potential to alleviate the substantial medical and psychosocial burdens of the disease.

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“…Biochemical in vitro analysis showed normal restoration of thrombin generation, and no discrepancy between 1‐stage activated partial thromboplastin time‐based and chromogenic assays. A further Phase 3 study is still under recruitment for PUPs (Liesner et al , ), however the participation rate had not yet reached the stage of 50 exposure days to inform on inhibitor rates compared with other currently licensed products.…”

Section: Factor Concentratesmentioning

confidence: 99%

Recent advances in developing specific therapies for haemophilia

2018

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Haemophilia therapy has undergone very rapid evolution in the last 10 years. The major limitation of current replacement therapy is the short half-life of factors VIII and IX. These half-lives have been extended by the addition of various moieties, allowing less frequent infusion regimens. Entirely novel approaches have also entered the clinic, including a bispecific antibody that mimics factor VIII and strategies that rebalance the haemostatic mechanism by reducing antithrombin through inhibition of synthesis. These two treatments are available by subcutaneous injection at infrequent intervals and both can be used in patients with neutralising antibodies (inhibitors). Finally, a cure may be on the horizon with preliminary evidence of success for gene therapy in haemophilia B and A.

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Inhibitor Development in Previously Untreated Patients with Severe Hemophilia a Treated with Nuwiq®, a New Generation Recombinant FVIII of Human Origin

Cited by 4 publications

References 0 publications

Current and emerging factor VIII replacement products for hemophilia A

Current and emerging factor VIII replacement products for hemophilia A

Protein-Engineered Coagulation Factors for Hemophilia Gene Therapy

Recent advances in developing specific therapies for haemophilia

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