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Literature DB >> 25406352

The intron-22-inverted F8 locus permits factor VIII synthesis: explanation for low inhibitor risk and a role for pharmacogenomics.

Zuben E Sauna¹, Jay N Lozier², Carol K Kasper³, Chen Yanover⁴, Timothy Nichols⁵, Tom E Howard⁶.

Abstract

Intron-22-inversion patients express the entire Factor VIII (FVIII)-amino-acid sequence intracellularly as 2 non-secreted polypeptides and have a positive "intracellular (I)-FVIII-CRM" status. Mutations conferring a positive I-FVIII-CRM status are associated with low inhibitor risk and are pharmacogenetically relevant because inhibitor risk may be affected by the nature of the therapeutic FVIII-protein (tFVIII), the affinity of any tFVIII-derived foreign peptide (tFVIII-fp) for any HLA class-II isomer (HLA-II) comprising individual major histocompatibility complex (MHC) repertoires, and the stability of any tFVIII-fp/HLA-II complex. We hypothesize that mutations conferring a completely or substantially negative I-FVIII-CRM status are pharmacogenetically irrelevant because inhibitor risk is high with any tFVIII and individual MHC repertoire.

Entities: Gene Species

Mesh：

Substances：

Year: 2014 PMID： 25406352 PMCID： PMC4287634 DOI： 10.1182/blood-2013-12-530113

Source DB: PubMed Journal: Blood ISSN： 0006-4971 Impact factor: 22.113

31 in total

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Review 6. Inhibitor development in correlation to factor VIII genotypes.

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7. Factor VIII gene (F8) mutation and risk of inhibitor development in nonsevere hemophilia A.

Authors: Corien L Eckhardt; Alice S van Velzen; Marjolein Peters; Jan Astermark; Paul P Brons; Giancarlo Castaman; Marjon H Cnossen; Natasja Dors; Carmen Escuriola-Ettingshausen; Karly Hamulyak; Daniel P Hart; Charles R M Hay; Saturnino Haya; Waander L van Heerde; Cedric Hermans; Margareta Holmström; Victor Jimenez-Yuste; Russell D Keenan; Robert Klamroth; Britta A P Laros-van Gorkom; Frank W G Leebeek; Ri Liesner; Anne Mäkipernaa; Christoph Male; Evelien Mauser-Bunschoten; Maria G Mazzucconi; Simon McRae; Karina Meijer; Michael Mitchell; Massimo Morfini; Marten Nijziel; Johannes Oldenburg; Kathelijne Peerlinck; Pia Petrini; Helena Platokouki; Sylvia E Reitter-Pfoertner; Elena Santagostino; Piercarla Schinco; Frans J Smiers; Berthold Siegmund; Annarita Tagliaferri; Thynn T Yee; Pieter Willem Kamphuisen; Johanna G van der Bom; Karin Fijnvandraat
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8. F8 haplotype and inhibitor risk: results from the Hemophilia Inhibitor Genetics Study (HIGS) Combined Cohort.

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Journal: PLoS Comput Biol Date: 2013-05-16 Impact factor: 4.475

10. Endogenous factor VIII synthesis from the intron 22-inverted F8 locus may modulate the immunogenicity of replacement therapy for hemophilia A.

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Review 3. Innovative Approaches for Immune Tolerance to Factor VIII in the Treatment of Hemophilia A.

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4. Safety and efficacy of turoctocog alfa in the prevention and treatment of bleeds in previously untreated paediatric patients with severe haemophilia A: Results from the guardian 4 multinational clinical trial.

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5. In situ genetic correction of F8 intron 22 inversion in hemophilia A patient-specific iPSCs.

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5 in total