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Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template

Adeno-associated virus (AAV)-based vectors are considered efficient and safe gene delivery systems in gene therapy. We combined two guide RNA genes, Cas9, and a self-linearizing repair template in one vector (AIO-SL) to correct fumarylacetoacetate hydrolase (FAH) deficiency in mice. The vector genom...

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Autores principales: Krooss, Simon Alexander, Dai, Zhen, Schmidt, Florian, Rovai, Alice, Fakhiri, Julia, Dhingra, Akshay, Yuan, Qinggong, Yang, Taihua, Balakrishnan, Asha, Steinbrück, Lars, Srivaratharajan, Sangar, Manns, Michael Peter, Schambach, Axel, Grimm, Dirk, Bohne, Jens, Sharma, Amar Deep, Büning, Hildegard, Ott, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6941859/
https://www.ncbi.nlm.nih.gov/pubmed/31887661
http://dx.doi.org/10.1016/j.isci.2019.100764
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author Krooss, Simon Alexander
Dai, Zhen
Schmidt, Florian
Rovai, Alice
Fakhiri, Julia
Dhingra, Akshay
Yuan, Qinggong
Yang, Taihua
Balakrishnan, Asha
Steinbrück, Lars
Srivaratharajan, Sangar
Manns, Michael Peter
Schambach, Axel
Grimm, Dirk
Bohne, Jens
Sharma, Amar Deep
Büning, Hildegard
Ott, Michael
author_facet Krooss, Simon Alexander
Dai, Zhen
Schmidt, Florian
Rovai, Alice
Fakhiri, Julia
Dhingra, Akshay
Yuan, Qinggong
Yang, Taihua
Balakrishnan, Asha
Steinbrück, Lars
Srivaratharajan, Sangar
Manns, Michael Peter
Schambach, Axel
Grimm, Dirk
Bohne, Jens
Sharma, Amar Deep
Büning, Hildegard
Ott, Michael
author_sort Krooss, Simon Alexander
collection PubMed
description Adeno-associated virus (AAV)-based vectors are considered efficient and safe gene delivery systems in gene therapy. We combined two guide RNA genes, Cas9, and a self-linearizing repair template in one vector (AIO-SL) to correct fumarylacetoacetate hydrolase (FAH) deficiency in mice. The vector genome of 5.73 kb was packaged into VP2-depleted AAV particles (AAV2/8(ΔVP2)), which, however, did not improve cargo capacity. Reprogrammed hepatocytes were treated with AIO-SL.AAV2(ΔVP2) and subsequently transplanted, resulting in large clusters of FAH-positive hepatocytes. Direct injection of AIO-SL.AAV8(ΔVP2) likewise led to FAH expression and long-term survival. The AIO-SL vector achieved an ∼6-fold higher degree of template integration than vectors without template self-linearization. Subsequent analysis revealed that AAV8 particles, in contrast to AAV2, incorporate oversized genomes distinctly greater than 5.2 kb. Finally, our AAV8-based vector represents a promising tool for gene editing strategies to correct monogenic liver diseases requiring (large) fragment removal and/or simultaneous sequence replacement.
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spelling pubmed-69418592020-01-06 Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template Krooss, Simon Alexander Dai, Zhen Schmidt, Florian Rovai, Alice Fakhiri, Julia Dhingra, Akshay Yuan, Qinggong Yang, Taihua Balakrishnan, Asha Steinbrück, Lars Srivaratharajan, Sangar Manns, Michael Peter Schambach, Axel Grimm, Dirk Bohne, Jens Sharma, Amar Deep Büning, Hildegard Ott, Michael iScience Article Adeno-associated virus (AAV)-based vectors are considered efficient and safe gene delivery systems in gene therapy. We combined two guide RNA genes, Cas9, and a self-linearizing repair template in one vector (AIO-SL) to correct fumarylacetoacetate hydrolase (FAH) deficiency in mice. The vector genome of 5.73 kb was packaged into VP2-depleted AAV particles (AAV2/8(ΔVP2)), which, however, did not improve cargo capacity. Reprogrammed hepatocytes were treated with AIO-SL.AAV2(ΔVP2) and subsequently transplanted, resulting in large clusters of FAH-positive hepatocytes. Direct injection of AIO-SL.AAV8(ΔVP2) likewise led to FAH expression and long-term survival. The AIO-SL vector achieved an ∼6-fold higher degree of template integration than vectors without template self-linearization. Subsequent analysis revealed that AAV8 particles, in contrast to AAV2, incorporate oversized genomes distinctly greater than 5.2 kb. Finally, our AAV8-based vector represents a promising tool for gene editing strategies to correct monogenic liver diseases requiring (large) fragment removal and/or simultaneous sequence replacement. Elsevier 2019-12-12 /pmc/articles/PMC6941859/ /pubmed/31887661 http://dx.doi.org/10.1016/j.isci.2019.100764 Text en © 2019 The Author(s) http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Krooss, Simon Alexander
Dai, Zhen
Schmidt, Florian
Rovai, Alice
Fakhiri, Julia
Dhingra, Akshay
Yuan, Qinggong
Yang, Taihua
Balakrishnan, Asha
Steinbrück, Lars
Srivaratharajan, Sangar
Manns, Michael Peter
Schambach, Axel
Grimm, Dirk
Bohne, Jens
Sharma, Amar Deep
Büning, Hildegard
Ott, Michael
Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title_full Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title_fullStr Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title_full_unstemmed Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title_short Ex Vivo/In vivo Gene Editing in Hepatocytes Using “All-in-One” CRISPR-Adeno-Associated Virus Vectors with a Self-Linearizing Repair Template
title_sort ex vivo/in vivo gene editing in hepatocytes using “all-in-one” crispr-adeno-associated virus vectors with a self-linearizing repair template
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6941859/
https://www.ncbi.nlm.nih.gov/pubmed/31887661
http://dx.doi.org/10.1016/j.isci.2019.100764
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