Pharmacokinetic analysis identifies a factor VIII immunogenicity threshold after AAV gene therapy in hemophilia A mice

Lundgren, Taran S.; Denning, Gabriela; Stowell, Sean R.; Spencer, H. Trent; Doering, Christopher B.

doi:10.1182/bloodadvances.2021006359

Cited by 5 publications

(3 citation statements)

References 70 publications

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“…5d ). Consistent with prior work 25,48,49 , studies in immune-competent HA/C57BL/6 mice challenged with recombinant FVIII ( Extended Data Fig. 4 a-c) or AAV-mediated FVIII expression ( Extended Data Fig.…”

Section: Resultssupporting

confidence: 88%

“…These experiments were also designed to assess if there were any differences in longitudinal pharmacokinetics of FVIII-WT and FVIII-QQ expression. HA/CD4KO mice were used because immune- competent C57BL/6 mice mount a robust antibody response to human FVIII expression 25 . Animals were assigned to the mild HA (0.05 to <0.4 nM), normal (0.4 to <1.5 nM) and elevated FVIII (>1.5 to 3 nM) cohorts based on their steady-state week 8 plasma FVIII antigen ( Fig.…”

Section: Resultsmentioning

confidence: 99%

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Overcoming Hemophilia A Gene Therapy Limitations with an Enhanced Function Factor VIII Variant

Sternberg,

Martos-Rus,

Davidson

et al. 2024

Preprint

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Durable factor VIII (FVIII) expression that normalizes hemostasis is an unrealized goal of hemophilia A adeno-associated virus (AAV)-mediated gene therapy. Trials with initial normal FVIII activity observed unexplained year-over-year declines in expression while others reported low-level, stable FVIII expression inadequate to restore normal hemostasis. Here we demonstrate that mice recapitulate FVIII expression-level-dependent loss of plasma FVIII levels due to declines in vector copy number. We show that an enhanced function FVIII variant (FVIII-R336Q/R562Q; FVIII-QQ), resistant to inactivation by protein C, normalizes hemostasis at below-normal expression levels without evidence of prothrombotic risk in hemophilia A mice. These data support that FVIII-QQ may restore normal FVIII function at low-levels of expression to permit durability using low AAV vector doses to minimize dose-dependent AAV toxicities. This work informs the mechanism of FVIII durability after AAV gene transfer and supports that incorporating the FVIII-QQ transgene may safely overcome current hemophilia A gene therapy limitations.

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Section: Resultssupporting

confidence: 88%

Section: Resultsmentioning

confidence: 99%

Overcoming Hemophilia A Gene Therapy Limitations with an Enhanced Function Factor VIII Variant

Sternberg,

Martos-Rus,

Davidson

et al. 2024

Preprint

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show abstract

“…Despite the limitations of the predictive value of preclinical immunogenicity testing, progress has been made in developing the principles of safe and effective genetic drug design in animal models. 73 In June 2022, the European Medicines Agency has recommended granting a conditional marketing authorization in the European Union for roxaparvovec valoctocogene gene therapy for the treatment of severe hemophilia A in adults who do not have factor VIII inhibitors or antibodies against adeno-associated virus serotype 5 (AAV5). Several clinical trials are currently investigating the safety and efficacy of gene therapy in hemophilia A (NCT05454774) and hemophilia B (NCT05203679).…”

Section: New Perspectives In the Approach And Management Of Patients ...mentioning

confidence: 99%

Hemophilic Arthropathy: Barriers to Early Diagnosis and Management

Cuesta‐Barriuso¹,

Donoso-Úbeda²,

Meroño-Gallut³

et al. 2022

JBM

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Hemophilia is a congenital coagulopathy characterized by a deficiency of one of the clotting factors. It is characterized by the development of hematomas and hemarthrosis, either spontaneously or after minor trauma. The recurrence of hemarthroses leads to progressive and degenerative joint damage from childhood (hemophilic arthropathy). This arthropathy is characterized by disabling physical effects that limit the functionality and quality of life of these patients. Medical progress achieved over the last decade in the drug treatment of hemophilia has improved the medium and long-term prospects of patients with more effective and long-lasting drugs. The universal use of safer, more effective and prolonged prophylactic treatments may promote the prevention of bleeding, and also therefore, of the development of hemarthrosis and joint damage. A number of imaging instruments have been developed for the assessment of hemarthrosis and hemophilic arthropathy, using ultrasound, magnetic resonance imaging and simple radiology. Different physical examination scores and questionnaires allow the assessment of joint health, self-perceived activity and functionality of patients with hemophilia. The approach to these patients should be interdisciplinary. Assessment of the processes that affect pain in these patients and the development of pain education models should be implemented. Expert advice and information to patients with hemophilia should be based on individual functional prevention diagnoses, advice on available therapies and sports practice, as well as health recommendations.

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A review of the rationale for gene therapy for hemophilia A with inhibitors: one-shot tolerance and treatment?

Valentino¹,

Ozelo²,

Herzog³

et al. 2023

Journal of Thrombosis and Haemostasis

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Pharmacokinetic analysis identifies a factor VIII immunogenicity threshold after AAV gene therapy in hemophilia A mice

Cited by 5 publications

References 70 publications

Overcoming Hemophilia A Gene Therapy Limitations with an Enhanced Function Factor VIII Variant

Overcoming Hemophilia A Gene Therapy Limitations with an Enhanced Function Factor VIII Variant

Hemophilic Arthropathy: Barriers to Early Diagnosis and Management

A review of the rationale for gene therapy for hemophilia A with inhibitors: one-shot tolerance and treatment?

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