Title (en)
CRISPR/Cas9-Mediated Targeting of BPV-1-Transformed Primary Equine Sarcoid Fibroblasts
Language
English
Description (en)
Equine sarcoids (EqS) are fibroblast-derived skin tumors associated with bovine papillomavirus 1 and 2 (BPV-1 and -2). Based on Southern blotting, the BPV-1 genome was not found to be integrated in the host cell genome, suggesting that EqS pathogenesis does not result from insertional mutagenesis. Hence, CRISPR/Cas9 implies an interesting tool for selectively targeting BPV-1 episomes or genetically anchored suspected host factors. To address this in a proof-of-concept study, we confirmed the exclusive episomal persistence of BPV-1 in EqS using targeted locus amplification (TLA). To investigate the CRISPR/Cas9-mediated editing of BPV-1 episomes, primary equine fibroblast cultures were established and characterized. In the EqS fibroblast cultures, CRISPR-mediated targeting of the episomal E5 and E6 oncogenes as well as the BPV-1 long control region was successful and resulted in a pronounced reduction of the BPV-1 load. Moreover, the deletion of the equine Vimentin (VIM), which is highly expressed in EqS, considerably decreased the number of BPV-1 episomes. Our results suggest CRISPR/Cas9-based gene targeting may serve as a tool to help further unravel the biology of EqS pathogenesis.
Keywords (en)
Bovine Papillomavirus Type-1; Vimentin Intermediate-Filaments; In-Vitro; Gene-Expression; Dna; Cells; Vivo; E6; Establishment; Inactivation
DOI
10.3390/v15091942
Author of the digital object
Anne Monod (University of Bern)
Kerstin Hahn (University of Bern)
Sven Rottenberg (University of Bern)
Vinzenz Gerber (University of Bern)
Christian Wenker (Zoo Basel)
Denise Howald (University of Bern)
Maarten Haspeslagh (Ghent University)
Christoph Koch (University of Bern)
Christoph Jindra (University of Veterinary Medicine Vienna)
Format
application/pdf
Size
1.0 MB
Licence Selected
CC BY 4.0 International
Type of publication
Article
Name of Publication (en)
Viruses
Pages or Volume
13
Volume
15
Number
9
Publisher
MDPI
Publication Date
2023
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- DetailsObject typePDFDocumentFormatapplication/pdfCreated26.02.2024 10:42:09
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