A Small-Molecule-Responsive Riboswitch Enables Conditional Induction of Viral Vector-Mediated Gene Expression in Mice

Strobel, Benjamin; Düchs, Matthias; Blazevic, Dragica; Rechtsteiner, Philipp; Braun, Clemens; Baum-Kroker, Katja S.; Schmid, Bernhard; Ciossek, Thomas; Gottschling, Dirk; Hartig, Jörg S.; Kreuz, Sebastian

doi:10.1021/acssynbio.9b00410

Cited by 35 publications

(40 citation statements)

References 50 publications

(89 reference statements)

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“…We used AAV2, AAV8, AAV9, AAV2.7m8 (Dalkara et al, 2013), ShH10 (Klimczak et al, 2009), and AAV2.NN, AAV2.GL (Pavlou et al, 2021) with the ss expression cassettes ss-CMV-eGFP-SV40poly(A), ss-CMV-anti-FITC, or sc-CMV-eGFP-SV40poly(A) (Strobel et al, 2020), flanked by AAV2-derived inverted terminal repeats. AAV vectors were prepared as in Strobel et al (2019): HEK 293-H cells were cultured in DMEM + GlutaMAX-I + 10% FCS (Thermo Fisher Scientific) and transfected as previously described (Strobel et al, 2015).…”

Section: Aav Vectorsmentioning

confidence: 99%

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

et al. 2021

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Gene therapies using adeno-associated viruses (AAVs) are among the most promising strategies to treat or even cure hereditary and acquired retinal diseases. However, the development of new efficient AAV vectors is slow and costly, largely because of the lack of suitable non-clinical models. By faithfully recreating structure and function of human tissues, human induced pluripotent stem cell (iPSC)derived retinal organoids could become an essential part of the test cascade addressing translational aspects. Organ-on-chip (OoC) technology further provides the capability to recapitulate microphysiological tissue environments as well as a precise control over structural and temporal parameters. By employing our recently developed retina on chip that merges organoid and OoC technology, we analyzed the efficacy, kinetics, and cell tropism of seven first-and second-generation AAV vectors. The presented data demonstrate the potential of iPSC-based OoC models as the next generation of screening platforms for future gene therapeutic studies.

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Section: Aav Vectorsmentioning

confidence: 99%

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

et al. 2021

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“…One tetracycline aptazyme, Tc40, enabled over 20-fold suppression in human cells and also achieved 7-fold suppression of an AAVdelivered transgene through oral administration of tetracycline in a mouse model. Strobel et al also recently demonstrated 15-fold induction of an AAV-delivered transgene in mice using a tetracycline-regulated aptazyme on-switch developed through a similar rational design and testing approach [154]. This result also represents a rare case in which switch performance was higher in an animal model than in previous results in cell culture [136].…”

Section: Improving the Function Of Aptazyme Riboswitchesmentioning

confidence: 91%

Riboswitches for Controlled Expression of Therapeutic Transgenes Delivered by Adeno-Associated Viral Vectors

Tickner

Farzan

2021

Pharmaceuticals

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Vectors developed from adeno-associated virus (AAV) are powerful tools for in vivo transgene delivery in both humans and animal models, and several AAV-delivered gene therapies are currently approved for clinical use. However, AAV-mediated gene therapy still faces several challenges, including limited vector packaging capacity and the need for a safe, effective method for controlling transgene expression during and after delivery. Riboswitches, RNA elements which control gene expression in response to ligand binding, are attractive candidates for regulating expression of AAV-delivered transgene therapeutics because of their small genomic footprints and non-immunogenicity compared to protein-based expression control systems. In addition, the ligand-sensing aptamer domains of many riboswitches can be exchanged in a modular fashion to allow regulation by a variety of small molecules, proteins, and oligonucleotides. Riboswitches have been used to regulate AAV-delivered transgene therapeutics in animal models, and recently developed screening and selection methods allow rapid isolation of riboswitches with novel ligands and improved performance in mammalian cells. This review discusses the advantages of riboswitches in the context of AAV-delivered gene therapy, the subsets of riboswitch mechanisms which have been shown to function in human cells and animal models, recent progress in riboswitch isolation and optimization, and several examples of AAV-delivered therapeutic systems which might be improved by riboswitch regulation.

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“…AAV2, AAV8, AAV9, AAV2.7m8 (Dalkara et al, 2013), ShH10 (Klimczak et al, 2009), and AAV2.NN, AAV2.GL (Pavlou et al, 2021) with the single stranded (ss) expression cassettes; ss-CMV-eGFP-SV40polyA, ss-CMV-antiFITC or self complementary (sc) sc-CMV-eGFP-SV40polyA, (Strobel et al, 2020) flanked by AAV2-derived inverted terminal repeats were applied. AAV vectors were prepared as previously described (Strobel et al, 2019).…”

Section: Methodsmentioning

confidence: 99%

Human stem cell-based retina-on-chip as new translational model for validation of AAV retinal gene therapy vectors

Achberger

Cipriano

Duechs

et al. 2021

Preprint

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Gene therapies using adeno-associated viruses (AAVs) are amongst the most promising strategies to treat or even cure hereditary and acquired retinal diseases. However, the development of new efficient AAV vectors is slow and costly, largely because of the lack of suitable non-clinical models. By faithfully recreating structure and function of human tissues, human induced pluripotent stem cell (iPSC)-derived retinal organoids could become an essential part of the test cascade addressing translational aspects. Organ-on-Chip (OoC) technology further provides the capability to recapitulate microphysiological tissue environments as well as a precise control over structural and temporal parameters. By employing our recently developed Retina-on-chip that merges organoid and OoC-technology, we analyzed the efficacy, kinetics and cell tropism of seven first and second generation AAV vectors. The presented data demonstrate the potential of iPSC-based OoC models as the next generation of screening platforms for future gene therapeutic studies.

show abstract

A Small-Molecule-Responsive Riboswitch Enables Conditional Induction of Viral Vector-Mediated Gene Expression in Mice

Cited by 35 publications

References 50 publications

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

Human stem cell-based retina on chip as new translational model for validation of AAV retinal gene therapy vectors

Riboswitches for Controlled Expression of Therapeutic Transgenes Delivered by Adeno-Associated Viral Vectors

Human stem cell-based retina-on-chip as new translational model for validation of AAV retinal gene therapy vectors

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