Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy

Gene therapy using adeno-associated virus (AAV)-based vectors has become a realistic therapeutic option for hemophilia. We examined the potential of a novel engineered liver-tropic AAV3B-based vector, AAV.GT5, for hemophilia B gene therapy. In vitro transduction with AAV.GT5 in human hepatocytes was...

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Autores principales: Kashiwakura, Yuji, Endo, Kazuhiro, Ugajin, Atsushi, Kikuchi, Tomohiro, Hishikawa, Shuji, Nakamura, Hitoyasu, Katakai, Yuko, Baatartsogt, Nemekhbayar, Hiramoto, Takafumi, Hayakawa, Morisada, Kamoshita, Nobuhiko, Yamazaki, Shoji, Kume, Akihiro, Mori, Harushi, Sata, Naohiro, Sakata, Yoichi, Muramatsu, Shin-ichi, Ohmori, Tsukasa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society of Gene & Cell Therapy 2023
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10491835/
https://www.ncbi.nlm.nih.gov/pubmed/37693948
http://dx.doi.org/10.1016/j.omtm.2023.08.016
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author Kashiwakura, Yuji
Endo, Kazuhiro
Ugajin, Atsushi
Kikuchi, Tomohiro
Hishikawa, Shuji
Nakamura, Hitoyasu
Katakai, Yuko
Baatartsogt, Nemekhbayar
Hiramoto, Takafumi
Hayakawa, Morisada
Kamoshita, Nobuhiko
Yamazaki, Shoji
Kume, Akihiro
Mori, Harushi
Sata, Naohiro
Sakata, Yoichi
Muramatsu, Shin-ichi
Ohmori, Tsukasa
author_facet Kashiwakura, Yuji
Endo, Kazuhiro
Ugajin, Atsushi
Kikuchi, Tomohiro
Hishikawa, Shuji
Nakamura, Hitoyasu
Katakai, Yuko
Baatartsogt, Nemekhbayar
Hiramoto, Takafumi
Hayakawa, Morisada
Kamoshita, Nobuhiko
Yamazaki, Shoji
Kume, Akihiro
Mori, Harushi
Sata, Naohiro
Sakata, Yoichi
Muramatsu, Shin-ichi
Ohmori, Tsukasa
author_sort Kashiwakura, Yuji
collection PubMed
description Gene therapy using adeno-associated virus (AAV)-based vectors has become a realistic therapeutic option for hemophilia. We examined the potential of a novel engineered liver-tropic AAV3B-based vector, AAV.GT5, for hemophilia B gene therapy. In vitro transduction with AAV.GT5 in human hepatocytes was more than 100 times higher than with AAV-Spark100, another bioengineered vector used in a clinical trial. However, liver transduction following intravenous injection of these vectors was similar in mice with a humanized liver and in macaques. This discrepancy was due to the low recovery and short half-life of AAV.GT5 in blood, depending on the positive charge of the heparin-binding site in the capsid. Bypassing systemic clearance with the intra-hepatic vascular administration of AAV.GT5, but not AAV-Spark100, enhanced liver transduction in pigs and macaques. AAV.GT5 did not develop neutralizing antibodies (NAbs) in two of four animals, while AAV-Spark100 induced serotype-specific NAbs in all macaques tested (4 of 4). The NAbs produced after AAV-Spark100 administration were relatively serotype specific, and challenge with AAV.GT5 through the hepatic artery successfully boosted liver transduction in one animal previously administered AAV-Spark100. In summary, AAV.GT5 showed different vector kinetics and NAb induction compared with AAV-Spark100, and intra-hepatic vascular administration may minimize the vector dose required and vector dissemination.
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spelling pubmed-104918352023-09-10 Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy Kashiwakura, Yuji Endo, Kazuhiro Ugajin, Atsushi Kikuchi, Tomohiro Hishikawa, Shuji Nakamura, Hitoyasu Katakai, Yuko Baatartsogt, Nemekhbayar Hiramoto, Takafumi Hayakawa, Morisada Kamoshita, Nobuhiko Yamazaki, Shoji Kume, Akihiro Mori, Harushi Sata, Naohiro Sakata, Yoichi Muramatsu, Shin-ichi Ohmori, Tsukasa Mol Ther Methods Clin Dev Original Article Gene therapy using adeno-associated virus (AAV)-based vectors has become a realistic therapeutic option for hemophilia. We examined the potential of a novel engineered liver-tropic AAV3B-based vector, AAV.GT5, for hemophilia B gene therapy. In vitro transduction with AAV.GT5 in human hepatocytes was more than 100 times higher than with AAV-Spark100, another bioengineered vector used in a clinical trial. However, liver transduction following intravenous injection of these vectors was similar in mice with a humanized liver and in macaques. This discrepancy was due to the low recovery and short half-life of AAV.GT5 in blood, depending on the positive charge of the heparin-binding site in the capsid. Bypassing systemic clearance with the intra-hepatic vascular administration of AAV.GT5, but not AAV-Spark100, enhanced liver transduction in pigs and macaques. AAV.GT5 did not develop neutralizing antibodies (NAbs) in two of four animals, while AAV-Spark100 induced serotype-specific NAbs in all macaques tested (4 of 4). The NAbs produced after AAV-Spark100 administration were relatively serotype specific, and challenge with AAV.GT5 through the hepatic artery successfully boosted liver transduction in one animal previously administered AAV-Spark100. In summary, AAV.GT5 showed different vector kinetics and NAb induction compared with AAV-Spark100, and intra-hepatic vascular administration may minimize the vector dose required and vector dissemination. American Society of Gene & Cell Therapy 2023-08-22 /pmc/articles/PMC10491835/ /pubmed/37693948 http://dx.doi.org/10.1016/j.omtm.2023.08.016 Text en © 2023 The Author(s) https://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 Original Article
Kashiwakura, Yuji
Endo, Kazuhiro
Ugajin, Atsushi
Kikuchi, Tomohiro
Hishikawa, Shuji
Nakamura, Hitoyasu
Katakai, Yuko
Baatartsogt, Nemekhbayar
Hiramoto, Takafumi
Hayakawa, Morisada
Kamoshita, Nobuhiko
Yamazaki, Shoji
Kume, Akihiro
Mori, Harushi
Sata, Naohiro
Sakata, Yoichi
Muramatsu, Shin-ichi
Ohmori, Tsukasa
Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title_full Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title_fullStr Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title_full_unstemmed Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title_short Efficient gene transduction in pigs and macaques with the engineered AAV vector AAV.GT5 for hemophilia B gene therapy
title_sort efficient gene transduction in pigs and macaques with the engineered aav vector aav.gt5 for hemophilia b gene therapy
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10491835/
https://www.ncbi.nlm.nih.gov/pubmed/37693948
http://dx.doi.org/10.1016/j.omtm.2023.08.016
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