Gene therapy by integrating vectors is promising for monogenic liver diseases, especially in children where episomal vectors remain transient. However, reaching the therapeutic threshold with genome-integrating vectors is challenging. Therefore, we developed a method to expand hepatocytes bearing therapeutic transgenes. The common fever medicine acetaminophen becomes hepatotoxic via cytochrome p450 metabolism. Lentiviral vectors with transgenes linked in cis to a Cypor shRNA were administered to neonatal mice. Hepatocytes lacking the essential cofactor of Cyp enzymes, NADPH-cytochrome p450 reductase (Cypor), were selected in vivo by acetaminophen administration, replacing up to 50% of the hepatic mass. Acetaminophen treatment of the mice resulted in over 30-fold expansion of transgene-bearing hepatocytes and achieved therapeutic thresholds in hemophilia B and phenylketonuria. We conclude that therapeutically modified hepatocytes can be selected safely and efficiently in preclinical models with a transient regimen of moderately hepatotoxic acetaminophen.

Therapeutic liver repopulation by transient acetaminophen selection of gene-modified hepatocytes / Vonada, A.; Tiyaboonchai, A.; Nygaard, S.; Posey, J.; Peters, A. M.; Winn, S. R.; Cantore, A.; Naldini, L.; Harding, C. O.; Grompe, M.. - In: SCIENCE TRANSLATIONAL MEDICINE. - ISSN 1946-6234. - 13:597(2021). [10.1126/scitranslmed.abg3047]

Therapeutic liver repopulation by transient acetaminophen selection of gene-modified hepatocytes

Cantore A.;Naldini L.;
2021-01-01

Abstract

Gene therapy by integrating vectors is promising for monogenic liver diseases, especially in children where episomal vectors remain transient. However, reaching the therapeutic threshold with genome-integrating vectors is challenging. Therefore, we developed a method to expand hepatocytes bearing therapeutic transgenes. The common fever medicine acetaminophen becomes hepatotoxic via cytochrome p450 metabolism. Lentiviral vectors with transgenes linked in cis to a Cypor shRNA were administered to neonatal mice. Hepatocytes lacking the essential cofactor of Cyp enzymes, NADPH-cytochrome p450 reductase (Cypor), were selected in vivo by acetaminophen administration, replacing up to 50% of the hepatic mass. Acetaminophen treatment of the mice resulted in over 30-fold expansion of transgene-bearing hepatocytes and achieved therapeutic thresholds in hemophilia B and phenylketonuria. We conclude that therapeutically modified hepatocytes can be selected safely and efficiently in preclinical models with a transient regimen of moderately hepatotoxic acetaminophen.
2021
Inglese
American Association for the Advancement of Science
13
597
eabg3047
9
Pubblicato
https://www.science.org/doi/10.1126/scitranslmed.abg3047
Esperti anonimi
Internazionale
Goal 3: Good health and well-being
Goal 9: Industry, Innovation, and Infrastructure
Goal 17: Partnerships for the goals
Animals
Genetic Therapy
Liver
Mice
Transgenes
Acetaminophen
Hepatocytes
Therapeutic liver repopulation by transient acetaminophen selection of gene-modified hepatocytes / Vonada, A.; Tiyaboonchai, A.; Nygaard, S.; Posey, J.; Peters, A. M.; Winn, S. R.; Cantore, A.; Naldini, L.; Harding, C. O.; Grompe, M.. - In: SCIENCE TRANSLATIONAL MEDICINE. - ISSN 1946-6234. - 13:597(2021). [10.1126/scitranslmed.abg3047]
open
10
info:eu-repo/semantics/article
262
Vonada, A.; Tiyaboonchai, A.; Nygaard, S.; Posey, J.; Peters, A. M.; Winn, S. R.; Cantore, A.; Naldini, L.; Harding, C. O.; Grompe, M.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.11768/122346
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