Publikation: A Small-Molecule-Responsive Riboswitch Enables Conditional Induction of Viral Vector-Mediated Gene Expression in Mice
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Adeno-associated viral (AAV) vector-mediated gene therapy holds great potential for future medical applications. However, to facilitate safer and broader applicability and to enable patient-centric care, therapeutic protein expression should be controllable, ideally by an orally administered drug. The use of protein-based systems is considered rather undesirable, due to potential immunogenicity and the limited coding space of AAV. Ligand-dependent riboswitches, in contrast, are small and characterized by an attractive mode-of-action based on mRNA-self-cleavage, independent of coexpressed foreign protein. While a promising approach, switches available to date have only shown moderate potency in animals. In particular, ON-switches that induce transgene expression upon ligand administration so far have achieved rather disappointing results. Here we present the utilization of the previously described tetracycline-dependent ribozyme K19 for controlling AAV-mediated transgene expression in mice. Using this tool switch, we provide first proof for the feasibility of clinically desired key features, including multiorgan functionality, potent regulation (up to 15-fold induction), reversibility, and the possibility to fine-tune and repeatedly induce expression. The systematic assessment of ligand and reporter protein plasma levels further enabled the characterization of pharmacokinetic-pharmacodynamic relationships. Thus, our results strongly support future efforts to develop engineered riboswitches for applications in clinical gene therapy.
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STROBEL, Benjamin, Matthias J. DÜCHS, Dragica BLAZEVIC, Philipp RECHTSTEINER, Clemens BRAUN, Katja S. BAUM-KROKER, Bernhard SCHMID, Thomas CIOSSEK, Dirk GOTTSCHLING, Jörg S. HARTIG, Sebastian KREUZ, 2020. A Small-Molecule-Responsive Riboswitch Enables Conditional Induction of Viral Vector-Mediated Gene Expression in Mice. In: ACS Synthetic Biology. American Chemical Society (ACS). 2020, 9(6), pp. 1292-1305. eISSN 2161-5063. Available under: doi: 10.1021/acssynbio.9b00410BibTex
@article{Strobel2020Small-50392,
year={2020},
doi={10.1021/acssynbio.9b00410},
title={A Small-Molecule-Responsive Riboswitch Enables Conditional Induction of Viral Vector-Mediated Gene Expression in Mice},
number={6},
volume={9},
journal={ACS Synthetic Biology},
pages={1292--1305},
author={Strobel, Benjamin and Düchs, Matthias J. and Blazevic, Dragica and Rechtsteiner, Philipp and Braun, Clemens and Baum-Kroker, Katja S. and Schmid, Bernhard and Ciossek, Thomas and Gottschling, Dirk and Hartig, Jörg S. and Kreuz, Sebastian}
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<dcterms:abstract xml:lang="eng">Adeno-associated viral (AAV) vector-mediated gene therapy holds great potential for future medical applications. However, to facilitate safer and broader applicability and to enable patient-centric care, therapeutic protein expression should be controllable, ideally by an orally administered drug. The use of protein-based systems is considered rather undesirable, due to potential immunogenicity and the limited coding space of AAV. Ligand-dependent riboswitches, in contrast, are small and characterized by an attractive mode-of-action based on mRNA-self-cleavage, independent of coexpressed foreign protein. While a promising approach, switches available to date have only shown moderate potency in animals. In particular, ON-switches that induce transgene expression upon ligand administration so far have achieved rather disappointing results. Here we present the utilization of the previously described tetracycline-dependent ribozyme K19 for controlling AAV-mediated transgene expression in mice. Using this tool switch, we provide first proof for the feasibility of clinically desired key features, including multiorgan functionality, potent regulation (up to 15-fold induction), reversibility, and the possibility to fine-tune and repeatedly induce expression. The systematic assessment of ligand and reporter protein plasma levels further enabled the characterization of pharmacokinetic-pharmacodynamic relationships. Thus, our results strongly support future efforts to develop engineered riboswitches for applications in clinical gene therapy.</dcterms:abstract>
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