Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells

Programmable nucleases have enabled rapid and accessible genome engineering in eukaryotic cells and living organisms. However, their delivery into human blood cells can be challenging. Here, we have utilized “nanoblades,” a new technology that delivers a genomic cleaving agent into cells. These are...

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Autores principales: Gutierrez-Guerrero, Alejandra, Abrey Recalde, Maria Jimena, Mangeot, Philippe E., Costa, Caroline, Bernadin, Ornellie, Périan, Séverine, Fusil, Floriane, Froment, Gisèle, Martinez-Turtos, Adriana, Krug, Adrien, Martin, Francisco, Benabdellah, Karim, Ricci, Emiliano P., Giovannozzi, Simone, Gijsbers, Rik, Ayuso, Eduard, Cosset, François-Loïc, Verhoeyen, Els
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2021
Materias:
Genome Editing
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8525375/
https://www.ncbi.nlm.nih.gov/pubmed/34713246
http://dx.doi.org/10.3389/fgeed.2021.604371
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author Gutierrez-Guerrero, Alejandra
Abrey Recalde, Maria Jimena
Mangeot, Philippe E.
Costa, Caroline
Bernadin, Ornellie
Périan, Séverine
Fusil, Floriane
Froment, Gisèle
Martinez-Turtos, Adriana
Krug, Adrien
Martin, Francisco
Benabdellah, Karim
Ricci, Emiliano P.
Giovannozzi, Simone
Gijsbers, Rik
Ayuso, Eduard
Cosset, François-Loïc
Verhoeyen, Els
author_facet Gutierrez-Guerrero, Alejandra
Abrey Recalde, Maria Jimena
Mangeot, Philippe E.
Costa, Caroline
Bernadin, Ornellie
Périan, Séverine
Fusil, Floriane
Froment, Gisèle
Martinez-Turtos, Adriana
Krug, Adrien
Martin, Francisco
Benabdellah, Karim
Ricci, Emiliano P.
Giovannozzi, Simone
Gijsbers, Rik
Ayuso, Eduard
Cosset, François-Loïc
Verhoeyen, Els
author_sort Gutierrez-Guerrero, Alejandra
collection PubMed
description Programmable nucleases have enabled rapid and accessible genome engineering in eukaryotic cells and living organisms. However, their delivery into human blood cells can be challenging. Here, we have utilized “nanoblades,” a new technology that delivers a genomic cleaving agent into cells. These are modified murine leukemia virus (MLV) or HIV-derived virus-like particle (VLP), in which the viral structural protein Gag has been fused to Cas9. These VLPs are thus loaded with Cas9 protein complexed with the guide RNAs. Highly efficient gene editing was obtained in cell lines, IPS and primary mouse and human cells. Here, we showed that nanoblades were remarkably efficient for entry into human T, B, and hematopoietic stem and progenitor cells (HSPCs) thanks to their surface co-pseudotyping with baboon retroviral and VSV-G envelope glycoproteins. A brief incubation of human T and B cells with nanoblades incorporating two gRNAs resulted in 40 and 15% edited deletion in the Wiskott-Aldrich syndrome (WAS) gene locus, respectively. CD34(+) cells (HSPCs) treated with the same nanoblades allowed 30–40% exon 1 drop-out in the WAS gene locus. Importantly, no toxicity was detected upon nanoblade-mediated gene editing of these blood cells. Finally, we also treated HSPCs with nanoblades in combination with a donor-encoding rAAV6 vector resulting in up to 40% of stable expression cassette knock-in into the WAS gene locus. Summarizing, this new technology is simple to implement, shows high flexibility for different targets including primary immune cells of human and murine origin, is relatively inexpensive and therefore gives important prospects for basic and clinical translation in the area of gene therapy.
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spelling pubmed-85253752021-10-27 Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells Gutierrez-Guerrero, Alejandra Abrey Recalde, Maria Jimena Mangeot, Philippe E. Costa, Caroline Bernadin, Ornellie Périan, Séverine Fusil, Floriane Froment, Gisèle Martinez-Turtos, Adriana Krug, Adrien Martin, Francisco Benabdellah, Karim Ricci, Emiliano P. Giovannozzi, Simone Gijsbers, Rik Ayuso, Eduard Cosset, François-Loïc Verhoeyen, Els Front Genome Ed Genome Editing Programmable nucleases have enabled rapid and accessible genome engineering in eukaryotic cells and living organisms. However, their delivery into human blood cells can be challenging. Here, we have utilized “nanoblades,” a new technology that delivers a genomic cleaving agent into cells. These are modified murine leukemia virus (MLV) or HIV-derived virus-like particle (VLP), in which the viral structural protein Gag has been fused to Cas9. These VLPs are thus loaded with Cas9 protein complexed with the guide RNAs. Highly efficient gene editing was obtained in cell lines, IPS and primary mouse and human cells. Here, we showed that nanoblades were remarkably efficient for entry into human T, B, and hematopoietic stem and progenitor cells (HSPCs) thanks to their surface co-pseudotyping with baboon retroviral and VSV-G envelope glycoproteins. A brief incubation of human T and B cells with nanoblades incorporating two gRNAs resulted in 40 and 15% edited deletion in the Wiskott-Aldrich syndrome (WAS) gene locus, respectively. CD34(+) cells (HSPCs) treated with the same nanoblades allowed 30–40% exon 1 drop-out in the WAS gene locus. Importantly, no toxicity was detected upon nanoblade-mediated gene editing of these blood cells. Finally, we also treated HSPCs with nanoblades in combination with a donor-encoding rAAV6 vector resulting in up to 40% of stable expression cassette knock-in into the WAS gene locus. Summarizing, this new technology is simple to implement, shows high flexibility for different targets including primary immune cells of human and murine origin, is relatively inexpensive and therefore gives important prospects for basic and clinical translation in the area of gene therapy. Frontiers Media S.A. 2021-02-09 /pmc/articles/PMC8525375/ /pubmed/34713246 http://dx.doi.org/10.3389/fgeed.2021.604371 Text en Copyright © 2021 Gutierrez-Guerrero, Abrey Recalde, Mangeot, Costa, Bernadin, Périan, Fusil, Froment, Martinez-Turtos, Krug, Martin, Benabdellah, Ricci, Giovannozzi, Gijsbers, Ayuso, Cosset and Verhoeyen. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Genome Editing
Gutierrez-Guerrero, Alejandra
Abrey Recalde, Maria Jimena
Mangeot, Philippe E.
Costa, Caroline
Bernadin, Ornellie
Périan, Séverine
Fusil, Floriane
Froment, Gisèle
Martinez-Turtos, Adriana
Krug, Adrien
Martin, Francisco
Benabdellah, Karim
Ricci, Emiliano P.
Giovannozzi, Simone
Gijsbers, Rik
Ayuso, Eduard
Cosset, François-Loïc
Verhoeyen, Els
Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title_full Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title_fullStr Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title_full_unstemmed Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title_short Baboon Envelope Pseudotyped “Nanoblades” Carrying Cas9/gRNA Complexes Allow Efficient Genome Editing in Human T, B, and CD34(+) Cells and Knock-in of AAV6-Encoded Donor DNA in CD34(+) Cells
title_sort baboon envelope pseudotyped “nanoblades” carrying cas9/grna complexes allow efficient genome editing in human t, b, and cd34(+) cells and knock-in of aav6-encoded donor dna in cd34(+) cells
topic Genome Editing
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8525375/
https://www.ncbi.nlm.nih.gov/pubmed/34713246
http://dx.doi.org/10.3389/fgeed.2021.604371
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