Toward optimal therapy for inhibitors in hemophilia

Kempton, Christine L.; Meeks, Shannon L.

doi:10.1182/blood-2014-05-577643

Cited by 125 publications

(169 citation statements)

References 56 publications

(56 reference statements)

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“…New treatments to promote immune tolerance to FVIII in individuals with an inhibitor or at increased risk for inhibitor development are therefore badly needed. 1 To facilitate their development, a better understanding of the anti-FVIII immune response, particularly in those who have developed a high-titer inhibitor refractive to ITI therapy, is required. Severe HA subject GS1-56A had failed ITI therapy and his high-titer inhibitor had persisted for .10 years.…”

Section: Discussionmentioning

confidence: 99%

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T cells from hemophilia A subjects recognize the same HLA-restricted FVIII epitope with a narrow TCR repertoire

Ettinger

Paz

James³

et al. 2016

Blood

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• An HA subject with a multiexon F8 deletion showed a highly clonal response to 1 FVIII epitope via an immunodominant TCR.• The same HLA-DRA*01-DRB1*01:01-restricted FVIII epitope was recognized by T cells from 3 HA subjects.Factor VIII (FVIII)-neutralizing antibodies ("inhibitors") are a serious problem in hemophilia A (HA). The aim of this study was to characterize HLA-restricted T-cell responses from a severe HA subject with a persistent inhibitor and from 2 previously studied mild HA inhibitor subjects. Major histocompatibility complex II tetramers corresponding to both of the severe HA subject's HLA-DRA-DRB1 alleles were loaded with peptides spanning FVIII-A2, C1, and C2 domains. Interestingly, only 1 epitope was identified, in peptide FVIII [2194][2195][2196][2197][2198][2199][2200][2201][2202][2203][2204][2205][2206][2207][2208][2209][2210][2211][2212][2213] , and it was identical to the HLA-DRA*01-DRB1*01:01-restricted epitope recognized by the mild HA subjects. Multiple T-cell clones and polyclonal lines having different avidities for the peptide-loaded tetramer were isolated from all subjects. Only high-and medium-avidity T cells proliferated and secreted cytokines when stimulated with FVIII 2194-2213 . T-cell receptor b (TCRB) gene sequencing of 15 T-cell clones from the severe HA subject revealed that all high-avidity clones expressed the same TCRB gene. High-throughput immunosequencing of high-, medium-, and low-avidity cells sorted from a severe HA polyclonal line revealed that 94% of the high-avidity cells expressed the same TCRB gene as the high-avidity clones. TCRB sequencing of clones and lines from the mild HA subjects also identified a limited TCRB gene repertoire. These results suggest a limited number of epitopes in FVIII drive inhibitor responses and that the T-cell repertoires of FVIII-responsive T cells can be quite narrow. The limited diversity of both epitopes and TCRB gene usage suggests that targeting of specific epitopes and/or T-cell clones may be a promising approach to achieve tolerance to FVIII. (Blood. 2016; 128(16):2043-2054

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Section: Discussionmentioning

confidence: 99%

“…1 Inhibitors occur more frequently in severe than in mild or moderate HA. [2][3][4] Inhibitor risk is associated with genetic and nongenetic factors.…”

Section: Introductionmentioning

confidence: 99%

T cells from hemophilia A subjects recognize the same HLA-restricted FVIII epitope with a narrow TCR repertoire

Ettinger

Paz

James³

et al. 2016

Blood

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“…14 In addition, because the replacement factor is effectively a foreign protein, treatment is often associated with formation of inhibitory antibodies, 15,16 which necessitates using a different class of therapeutics termed "bypassing agents." 17 Bypassing agents increase thrombin generation through mechanisms independent of the intrinsic Xase complex, the most commonly used of which are fVIIa (NovoSeven), prothrombin concentrates, and FEIBA. However, these agents suffer from short half-lives and result in variable responses in patients.…”

Section: Introductionmentioning

confidence: 99%

Design and characterization of an APC-specific serpin for the treatment of hemophilia

Polderdijk

Adams

Ivanciu

et al. 2017

Blood

121

120

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“…This immune response to protein antigens can cause life-threatening anaphylaxis in severe cases [32]. Current clinical protocols of immune tolerance induction (ITI) require administration of high doses of blood clotting factor over a long period of time [33]. However, this clinical protocol is highly expensive and it does not guarantee the effective immune tolerance [1].…”

Section: Immune Modulationmentioning

confidence: 99%

Expression and functional evaluation of biopharmaceuticals made in plant chloroplasts

Zhang

Shanmugaraj

Daniell

2017

Current Opinion in Chemical Biology

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After approval of the first plant-made biopharmaceutical by FDA for human use, many protein drugs are now in clinical development. Within the last decade, significant advances have been made in expression of heterologous complex/large proteins in chloroplasts of edible plants using codon optimized human or viral genes. Furthermore, advances in quantification enable determination of in-planta drug dosage. Oral delivery of plastid-made biopharmaceuticals (PMB) is affordable because it eliminates prohibitively expensive fermentation, purification processes addressing major challenges of short shelf-life after cold storage. In this review, we discuss recent advances in PMBs against metabolic, inherited or infectious diseases, and also mechanisms of post-translational modifications (PTM) in order to increase our understanding of functional PMBs.

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Toward optimal therapy for inhibitors in hemophilia

Cited by 125 publications

References 56 publications

T cells from hemophilia A subjects recognize the same HLA-restricted FVIII epitope with a narrow TCR repertoire

T cells from hemophilia A subjects recognize the same HLA-restricted FVIII epitope with a narrow TCR repertoire

Design and characterization of an APC-specific serpin for the treatment of hemophilia

Expression and functional evaluation of biopharmaceuticals made in plant chloroplasts

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