Endogenous Factor VIII Synthesis from the Intron 22-inverted F8 Locus May Modulate the Immunogenicity of Replacement Therapy for Hemophilia A

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2013 Sep 17

PMID 24037092

Citations 27

Authors

Gouri Shankar Pandey

Chen Yanover

Lisa M Miller-Jenkins

Susan Garfield

Shelley A Cole

Joanne E Curran

Eric K Moses

Natalia Rydz

Vijaya Simhadri

Chava Kimchi-Sarfaty

David Lillicrap

Kevin R Viel

Teresa M Przytycka

Glenn F Pierce

Tom E Howard

Zuben E Sauna

Affiliations

Soon will be listed here.

Abstract

Neutralizing antibodies (inhibitors) to replacement factor VIII (FVIII, either plasma derived or recombinant) impair the effective management of hemophilia A. Individuals with hemophilia A due to major deletions of the FVIII gene (F8) lack antigenically cross-reactive material in their plasma ("CRM-negative"), and the prevalence of inhibitors in these individuals may be as high as 90%. Conversely, individuals with hemophilia A caused by F8 missense mutations are CRM-positive, and their overall prevalence of inhibitors is <10% (ref. 2). Individuals with the F8 intron 22 inversion (found in ∼50% of individuals with severe hemophilia A) have been grouped with the former on the basis of their genetic defect and CRM-negative status. However, only ∼20% of these individuals develop inhibitors. Here we demonstrate that the levels of F8 mRNA and intracellular FVIII protein in B lymphoblastoid cells and liver biopsies from individuals with the intron 22 inversion are comparable to those in healthy controls. These results support the hypothesis that most individuals with the intron 22 inversion are tolerized to FVIII and thus do not develop inhibitors. Furthermore, we developed a new pharmacogenetic algorithm that permits the stratification of inhibitor risk for individuals and subpopulations by predicting the immunogenicity of replacement FVIII using, as input, the number of putative T cell epitopes in the infused protein and the competence of major histocompatibility complex class II molecules to present such epitopes. This algorithm showed statistically significant accuracy in predicting the presence of inhibitors in 25 unrelated individuals with the intron 22 inversion.

Citing Articles

Prediction of the chance of successful immune tolerance induction in persons with severe hemophilia A and inhibitors: a clinical prediction model.

Oomen I, Abdi A, Camelo R, Callado F, Carvalho L, Calcaterra I Res Pract Thromb Haemost. 2024; 8(7):102580.

PMID: 39558913 PMC: 11570954. DOI: 10.1016/j.rpth.2024.102580.

Identification of the Efficient Enhancer Elements in FVIII-Padua for Gene Therapy Study of Hemophilia A.

Xiao R, Chen Y, Hu Z, Tang Q, Wang P, Zhou M Int J Mol Sci. 2024; 25(7).

PMID: 38612447 PMC: 11011560. DOI: 10.3390/ijms25073635.

A Scan of Pleiotropic Immune Mediated Disease Genes Identifies Novel Determinants of Baseline FVIII Inhibitor Status in Hemophilia-A.

Howard T, Almieda M, Diego V, Viel K, Luu B, Haack K Res Sq. 2023; .

PMID: 37886476 PMC: 10602130. DOI: 10.21203/rs.3.rs-3371095/v1.

A machine learning approach for identifying variables associated with risk of developing neutralizing antidrug antibodies to factor VIII.

Rawal A, Kidchob C, Ou J, Yogurtcu O, Yang H, Sauna Z Heliyon. 2023; 9(6):e16331.

PMID: 37251488 PMC: 10220358. DOI: 10.1016/j.heliyon.2023.e16331.

Hemophilia A subjects with an intron-22 gene inversion mutation show CD4 T-effector responses to multiple epitopes in FVIII.

Gunasekera D, Vir P, Karim A, Ragni M, Pratt K Front Immunol. 2023; 14:1128641.

PMID: 36936969 PMC: 10015889. DOI: 10.3389/fimmu.2023.1128641.

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