A Novel Platform for Immune Tolerance Induction in Hemophilia A Mice

Merlin, Simone; Cannizzo, Elvira S.; Borroni, Ester; Bruscaggin, Valentina; Schinco, Piercarla; Tulalamba, Warut; Chuah, Marinee; Arruda, Valder R.; VandenDriessche, Thierry; Prat, María; Valente, Guido; Follenzi, Antonia

doi:10.1016/j.ymthe.2017.04.029

Cited by 53 publications

(102 citation statements)

References 75 publications

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“…The latter can induce immune tolerance, although recent literature suggests that targeting LSEC, as compared to hepatocytes, may better induce tolerance, perhaps owing to their ability to promote induction of Treg. 5,6,12 Potential reasons for differences in immunogenicity of FVIII produced by varying cell types need to be better addressed.…”

Section: Certain Types Of Macrophages and Marginal Zone B Cells Have mentioning

confidence: 99%

“…Recombinant FVIII is made in various mammalian cell lines (none of which are endothelial cells) and current gene therapies target hepatocytes for FVIII expression. The latter can induce immune tolerance, although recent literature suggests that targeting LSEC, as compared to hepatocytes, may better induce tolerance, perhaps owing to their ability to promote induction of Treg …”

Section: Introductionmentioning

confidence: 99%

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The national blueprint for future basic and translational research to understand factor VIII immunogenicity: NHLBI State of the Science Workshop on factor VIII inhibitors

Meeks

Herzog

2019

Haemophilia

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Introduction Inhibitor formation against coagulation factor VIII (FVIII) is an unresolved serious problem in replacement therapy for the X‐linked bleeding disorder haemophilia A. Although FVIII inhibitors have been extensively studied, much of the basic mechanism of this immune response remains to be uncovered. Aim Within the NHLBI State of the Science Workshop on Factor VIII Inhibitors, Working Group 3 identified three scientific priorities for basic and translational research on FVIII inhibitor formation. Methods A larger list of potential areas of research was initially developed as a basis for subsequent prioritization. Each scientific goal was further evaluated based on required effort, potential impact, approach, methods, technologies and models. Results The three priorities include the following: activation signals and immune regulation that shape the response to FVIII (including innate immunity, microbiome, adaptive immunity and regulatory T cell studies in humans); utility of animal models and non‐animal approaches (in silico, genetic, single‐cell/sorted population “omics,” in vitro) to help predict inhibitor formation and identify novel therapeutics; and impact of the source of FVIII, its structure and von Willebrand factor on immunogenicity and tolerance. Conclusions Early interactions between FVIII and the immune system, biomarker development and studies in different patient groups (previously treated or untreated, with or without inhibitor formation, patients undergoing immune tolerance induction or gene therapy) deserve particular emphasis. Finally, linking basic to clinical studies, development of a repository for biospecimens and opportunities for interdisciplinary research training are important components to solving the urgent problem of inhibitor formation.

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Section: Certain Types Of Macrophages and Marginal Zone B Cells Have mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The national blueprint for future basic and translational research to understand factor VIII immunogenicity: NHLBI State of the Science Workshop on factor VIII inhibitors

Meeks

Herzog

2019

Haemophilia

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“…[11][12][13][14][15] The induction of immune tolerance to the coagulation factors after gene therapy is dependent on several variables. [11][12][13][14][15] The induction of immune tolerance to the coagulation factors after gene therapy is dependent on several variables.…”

Section: G Ene Ther Apymentioning

confidence: 99%

“…68 If FVIII or FIX is inadvertently expressed in APCs, the risk of inhibitory antibody development is increased, which prevents long-term expression and makes the gene therapy unsuccessful. 15 The immune tolerance that is induced by hepatic FVIII or FIX gene transfer by lentiviral vectors typically requires regulatory T-cell induction. 15 The immune tolerance that is induced by hepatic FVIII or FIX gene transfer by lentiviral vectors typically requires regulatory T-cell induction.…”

Section: γ-Retroviral and Lentiviral Vectorsmentioning

confidence: 99%

“…25,46 The use of hepatocyte-specific promoters can avoid expression in APCs and in this way result in long-term FIX expression. 15,24,35,71 We have shown that introducing a codon-optimized hyperactive FIX-R338L (Padua) gene with either integration-defective or integration-competent lentiviral vectors in haemophilia B mice could significantly augment FIX activity. 15,24,35,71 We have shown that introducing a codon-optimized hyperactive FIX-R338L (Padua) gene with either integration-defective or integration-competent lentiviral vectors in haemophilia B mice could significantly augment FIX activity.…”

Section: γ-Retroviral and Lentiviral Vectorsmentioning

confidence: 99%

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Haemophilia gene therapy: From trailblazer to gamechanger

2018

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Haemophilia is an attractive disease target for gene therapy that fostered the development of the field at large. The delivery of the clotting factor genes into the patients' cells could be accomplished using different types of gene delivery vehicles or vectors. Adeno-associated viral vectors (AAV) and lentiviral vectors represent some of the most promising gene delivery technologies that allow for a relatively efficient delivery of the therapeutic FVIII and FIX transgenes into the relevant target cells. To reduce the risks associated with insertional mutagenesis due to random vector integration, gene-editing approaches have also been considered based primarily on zinc finger nuclease (ZFN) and CRISPR/Cas. However, comprehensive analysis of off-target effects is still required. It is particularly encouraging that relatively stable therapeutic FVIII or FIX expression levels were reached in severe haemophilia patients in recent clinical trials after liver-directed AAV gene therapy. This success could be ascribed in part to improvements in vector design. In particular, clotting factor levels could be increased by codon optimization of coagulation factor transgenes. Alternatively, incorporation of a hyperactive gain-of-function R338L mutation (FIX Padua) in the FIX gene improved the overall efficacy. However, some patients still show transient liver toxicity, especially at high vector doses, possibly due to inflammatory immune responses, requiring the need for transient immunosuppression. The exact immune mechanisms are not fully understood, but may at least in some patients involve an AAV-capsid specific T cell response. Moreover, there is a need to identify the key factors that contribute to the interpatient variability in therapeutic efficacy and safety after gene therapy.

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Harnessing lentiviral vectors for in vivo gene therapy of liver metastases

Giacca,

Naldini,

Squadrito

2024

Clinical & Translational Med

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Liver metastases (LMS) commonly arise from gastrointestinal tumors, such as colorectal cancer (CRC) and pancreatic cancer (PDAC). The immunosuppressive environment of the liver favors cancer cell seeding and metastasis generation by impairing immune activation and promoting immune escape. In agreement with this observation, most pharmacological interventions, including recent immunotherapies, prove ineffective in the presence of LMS. For example, immunotherapeutic treatments, which are successful against melanoma, show reduced efficacy in the presence of LMS. 1 Thus, it is of pivotal importance to develop innovative therapeutic interventions that favor immune activation and unleash immune effector functions to eradicate LMS.To respond to this unmet clinical need, we developed a lentiviral vector (LV)-based in vivo gene therapy platform, which upon a single well-tolerated intravenous (i.v.) injection in mice, conveys expression of interferon-alpha (IFNα) to liver macrophages. 2 LVs are HIV-1-derived selfinactivating viral vectors, which do not replicate in the host upon cell transduction. Moreover, LVs efficiently transduce both proliferating as well as non-proliferating cells and integrate into the genome of the target cell enablingThis is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

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A Novel Platform for Immune Tolerance Induction in Hemophilia A Mice

Cited by 53 publications

References 75 publications

The national blueprint for future basic and translational research to understand factor VIII immunogenicity: NHLBI State of the Science Workshop on factor VIII inhibitors

The national blueprint for future basic and translational research to understand factor VIII immunogenicity: NHLBI State of the Science Workshop on factor VIII inhibitors

Haemophilia gene therapy: From trailblazer to gamechanger

Harnessing lentiviral vectors for in vivo gene therapy of liver metastases

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