Improved adeno-associated virus (AAV) serotype 1 and 5 vectors for gene therapy

Dwaipayan Sen; Balaji Balakrishnan; Nishanth Gabriel; Prachi Agrawal; Vaani Roshini; Rekha Samuel; Alok Srivastava; Giridhara R. Jayandharan

doi:10.1038/srep01832

Improved adeno-associated virus (AAV) serotype 1 and 5 vectors for gene therapy

Dwaipayan Sen, Balaji Balakrishnan, Nishanth Gabriel, Prachi Agrawal, Vaani Roshini, Rekha Samuel, Alok Srivastava, Giridhara R. Jayandharan

Division of Hematology & Oncology

Research output: Contribution to journal › Article › peer-review

41 Scopus citations

Abstract

Despite significant advancements with recombinant AAV2 or AAV8 vectors for liver directed gene therapy in humans, it is well-recognized that host and vector-related immune challenges need to be overcome for long-term gene transfer. To overcome these limitations, alternate AAV serotypes (1-10) are being rigorously evaluated. AAV5 is the most divergent (55% similarity vs. other serotypes) and like AAV1 vector is known to transduce liver efficiently. AAV1 and AAV5 vectors are also immunologically distinct by virtue of their low seroprevalence and minimal cross reactivity against pre-existing AAV2 neutralizing antibodies. Here, we demonstrate that targeted bio-engineering of these vectors, augment their gene expression in murine hepatocytes in vivo (up to 16-fold). These studies demonstrate the feasibility of the use of these novel AAV1 and AAV5 vectors for potential gene therapy of diseases like hemophilia.

Original language	English
Article number	1832
Journal	Scientific reports
Volume	6
DOIs	https://doi.org/10.1038/srep01832
State	Published - 2013

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abstract = "Despite significant advancements with recombinant AAV2 or AAV8 vectors for liver directed gene therapy in humans, it is well-recognized that host and vector-related immune challenges need to be overcome for long-term gene transfer. To overcome these limitations, alternate AAV serotypes (1-10) are being rigorously evaluated. AAV5 is the most divergent (55\% similarity vs. other serotypes) and like AAV1 vector is known to transduce liver efficiently. AAV1 and AAV5 vectors are also immunologically distinct by virtue of their low seroprevalence and minimal cross reactivity against pre-existing AAV2 neutralizing antibodies. Here, we demonstrate that targeted bio-engineering of these vectors, augment their gene expression in murine hepatocytes in vivo (up to 16-fold). These studies demonstrate the feasibility of the use of these novel AAV1 and AAV5 vectors for potential gene therapy of diseases like hemophilia.",

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AU - Sen, Dwaipayan

AU - Balakrishnan, Balaji

AU - Gabriel, Nishanth

AU - Agrawal, Prachi

AU - Roshini, Vaani

AU - Samuel, Rekha

AU - Srivastava, Alok

AU - Jayandharan, Giridhara R.

PY - 2013

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AB - Despite significant advancements with recombinant AAV2 or AAV8 vectors for liver directed gene therapy in humans, it is well-recognized that host and vector-related immune challenges need to be overcome for long-term gene transfer. To overcome these limitations, alternate AAV serotypes (1-10) are being rigorously evaluated. AAV5 is the most divergent (55% similarity vs. other serotypes) and like AAV1 vector is known to transduce liver efficiently. AAV1 and AAV5 vectors are also immunologically distinct by virtue of their low seroprevalence and minimal cross reactivity against pre-existing AAV2 neutralizing antibodies. Here, we demonstrate that targeted bio-engineering of these vectors, augment their gene expression in murine hepatocytes in vivo (up to 16-fold). These studies demonstrate the feasibility of the use of these novel AAV1 and AAV5 vectors for potential gene therapy of diseases like hemophilia.

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Improved adeno-associated virus (AAV) serotype 1 and 5 vectors for gene therapy

Abstract

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