Effects of FVIII immunity on hepatocyte and hematopoietic stem cell–directed gene therapy of murine hemophilia A

Lytle, Allison M; Brown, Harrison C.; Paik, Na Yoon; Knight, Kristopher A.; Wright, J. Fraser; Spencer, H. Trent; Doering, Christopher B.

doi:10.1038/mtm.2015.56

Cited by 22 publications

(37 citation statements)

References 60 publications

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“…In contrast to the canine model, reversal in hemophilia A mice by hepatic AAV gene transfer has been challenging [95]. This may reflect differences in generation of long-lived plasma cells between the two species in response to FVIII, which may be harder to suppress.…”

Section: Immune Tolerance Induction To the Transgene Product By LImentioning

confidence: 99%

“…This may reflect differences in generation of long-lived plasma cells between the two species in response to FVIII, which may be harder to suppress. However, preventive tolerance induction has been accomplished in the mice using optimized expression cassettes [84, 95, 96]. High levels of FVIII expression in hepatocytes has some potential for induction of a cellular stress response, which however does not appear to increase immunogenicity [96, 97].…”

Section: Immune Tolerance Induction To the Transgene Product By LImentioning

confidence: 99%

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Complexity of immune responses to AAV transgene products – Example of factor IX

Herzog

2019

Cellular Immunology

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After two decades of research, in vivo gene transfer with adeno-associated viral (AAV) vectors has now resulted in successful treatments and even cures for several human diseases. However, the potential for immune responses against the therapeutic gene products remains one of the concerns as this approach is broadened to more patients, diverse diseases, and target organs. Immune responses following gene transfer of coagulation factor IX (FIX) for the treatment of the bleeding disorder hemophilia B has been extensively investigated in multiple animal models. Findings from these studies have not only influenced clinical trial design but have broader implications for other diseases. The impact of vector design and dose, as well as target organ/route of administration on humoral and cellular immune responses are reviewed. Furthermore, the potential for tolerance induction by hepatic gene transfer or combination with immune modulation is discussed.

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Section: Immune Tolerance Induction To the Transgene Product By LImentioning

confidence: 99%

Section: Immune Tolerance Induction To the Transgene Product By LImentioning

confidence: 99%

Complexity of immune responses to AAV transgene products – Example of factor IX

Herzog

2019

Cellular Immunology

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“…The results are undoubtedly encouraging. Instead of liver-directed gene transfer, HSC-directed F8 gene transfer has been investigated and showed advantages in tackling pre-existing immunity [237]. Hence, the search for alternative approaches could address these limitations and expand our treatment options.…”

Section: Hemophiliamentioning

confidence: 99%

“…Efficient targeted integration of a F9 gene was also demonstrated by using a single HDAd vector simultaneously carrying CRISPR/Cas9 and a donor cassette [105]. Instead of liver-directed gene transfer, HSC-directed F8 gene transfer has been investigated and showed advantages in tackling pre-existing immunity [237]. We recently reported on an approach for HSCderived, erythroid-specific F8 production based on HDAd5/35++ vectors [151].…”

Section: Hemophiliamentioning

confidence: 99%

Adenovirus vectors in hematopoietic stem cell genome editing

Lieber

2019

FEBS Letters

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Genome editing of hematopoietic stem cells (HSCs) represents a therapeutic option for a number of hematological genetic diseases, as HSCs have the potential for self-renewal and differentiation into all blood cell lineages. This review presents advances of genome editing in HSCs utilizing adenovirus vectors as delivery vehicles. We focus on capsid-modified, helper-dependent adenovirus vectors that are devoid of all viral genes and therefore exhibit an improved safety profile. We discuss HSC genome engineering for several inherited disorders and infectious diseases including hemoglobinopathies, Fanconi anemia, hemophilia, and HIV-1 infection by ex vivo and in vivo editing in transgenic mice, nonhuman primates, as well as in human CD34 + cells. Mechanisms of therapeutic gene transfer including episomal expression of designer nucleases and base editors, transposase-mediated random integration, and targeted homology-directed repair triggered integration into selected genomic safe harbor loci are also reviewed.

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“…Drawbacks to the current hemophilia treatments have prompted researchers to seek alternatives, such as discovery of longer-acting factors that can be used at lower doses, utilization of non-factor therapies, and gene therapy. Gene therapy particularly is expected to be the key to curing hemophilia [34, 35]. …”

Section: Targeting Protein S In Hemophiliamentioning

confidence: 99%