Native and engineered tropism of vectors derived from a rare species D adenovirus serotype 43

Natalya Belousova; Galina Mikheeva; Chiyi Xiong; Loren J. Stagg; Mihai Gagea; Patricia S. Fox; Roland L. Bassett; John E. Ladbury; Michael B. Braun; Thilo Stehle; Chun Li; Victor Krasnykh

doi:10.18632/oncotarget.10800

Native and engineered tropism of vectors derived from a rare species D adenovirus serotype 43

Natalya Belousova, Galina Mikheeva, Chiyi Xiong, Loren J. Stagg, Mihai Gagea, Patricia S. Fox, Roland L. Bassett, John E. Ladbury, Michael B. Braun, Thilo Stehle, Chun Li, Victor Krasnykh

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

12 Scopus citations

Abstract

Unique molecular properties of species D adenoviruses (Ads)-the most diverse yet underexplored group of Ads-have been used to develop improved gene vectors. The low seroprevalence in humans of adenovirus serotype 43 (Ad43), an otherwise unstudied species D Ad, identified this rare serotype as an attractive new human gene therapy vector platform. Thus, in this study we wished to assess biological properties of Ad43 essential to its vectorization. We found that (1) Ad43 virions do not bind blood coagulation factor X and cause low random transduction upon vascular delivery; (2) they clear host tissues more quickly than do traditionally used Ad5 vectors; (3) Ad43 uses CD46 as primary receptor; (4) Ad43 can use integrins as alternative primary receptors. As the first step toward vectorization of Ad43, we demonstrated that the primary receptor specificity of the Ad43 fiber can be altered to achieve infection via Her2, an established oncotarget. Whereas this modification required use of the Ad5 fiber shaft, the presence of this domain in chimeric virions did not make them susceptible for neutralization by anti-Ad5 antibodies.

Original language	English (US)
Pages (from-to)	53414-53429
Number of pages	16
Journal	Oncotarget
Volume	7
Issue number	33
DOIs	https://doi.org/10.18632/oncotarget.10800
State	Published - Aug 1 2016

Keywords

Adenovirus
CD46
Serotype
Targeting
Tropism

ASJC Scopus subject areas

Oncology

MD Anderson CCSG core facilities

Biostatistics Resource Group

Access to Document

10.18632/oncotarget.10800

Cite this

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title = "Native and engineered tropism of vectors derived from a rare species D adenovirus serotype 43",

abstract = "Unique molecular properties of species D adenoviruses (Ads)-the most diverse yet underexplored group of Ads-have been used to develop improved gene vectors. The low seroprevalence in humans of adenovirus serotype 43 (Ad43), an otherwise unstudied species D Ad, identified this rare serotype as an attractive new human gene therapy vector platform. Thus, in this study we wished to assess biological properties of Ad43 essential to its vectorization. We found that (1) Ad43 virions do not bind blood coagulation factor X and cause low random transduction upon vascular delivery; (2) they clear host tissues more quickly than do traditionally used Ad5 vectors; (3) Ad43 uses CD46 as primary receptor; (4) Ad43 can use integrins as alternative primary receptors. As the first step toward vectorization of Ad43, we demonstrated that the primary receptor specificity of the Ad43 fiber can be altered to achieve infection via Her2, an established oncotarget. Whereas this modification required use of the Ad5 fiber shaft, the presence of this domain in chimeric virions did not make them susceptible for neutralization by anti-Ad5 antibodies.",

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author = "Natalya Belousova and Galina Mikheeva and Chiyi Xiong and Stagg, {Loren J.} and Mihai Gagea and Fox, {Patricia S.} and Bassett, {Roland L.} and Ladbury, {John E.} and Braun, {Michael B.} and Thilo Stehle and Chun Li and Victor Krasnykh",

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doi = "10.18632/oncotarget.10800",

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T1 - Native and engineered tropism of vectors derived from a rare species D adenovirus serotype 43

AU - Belousova, Natalya

AU - Mikheeva, Galina

AU - Xiong, Chiyi

AU - Stagg, Loren J.

AU - Gagea, Mihai

AU - Fox, Patricia S.

AU - Bassett, Roland L.

AU - Ladbury, John E.

AU - Braun, Michael B.

AU - Stehle, Thilo

AU - Li, Chun

AU - Krasnykh, Victor

PY - 2016/8/1

Y1 - 2016/8/1

N2 - Unique molecular properties of species D adenoviruses (Ads)-the most diverse yet underexplored group of Ads-have been used to develop improved gene vectors. The low seroprevalence in humans of adenovirus serotype 43 (Ad43), an otherwise unstudied species D Ad, identified this rare serotype as an attractive new human gene therapy vector platform. Thus, in this study we wished to assess biological properties of Ad43 essential to its vectorization. We found that (1) Ad43 virions do not bind blood coagulation factor X and cause low random transduction upon vascular delivery; (2) they clear host tissues more quickly than do traditionally used Ad5 vectors; (3) Ad43 uses CD46 as primary receptor; (4) Ad43 can use integrins as alternative primary receptors. As the first step toward vectorization of Ad43, we demonstrated that the primary receptor specificity of the Ad43 fiber can be altered to achieve infection via Her2, an established oncotarget. Whereas this modification required use of the Ad5 fiber shaft, the presence of this domain in chimeric virions did not make them susceptible for neutralization by anti-Ad5 antibodies.

AB - Unique molecular properties of species D adenoviruses (Ads)-the most diverse yet underexplored group of Ads-have been used to develop improved gene vectors. The low seroprevalence in humans of adenovirus serotype 43 (Ad43), an otherwise unstudied species D Ad, identified this rare serotype as an attractive new human gene therapy vector platform. Thus, in this study we wished to assess biological properties of Ad43 essential to its vectorization. We found that (1) Ad43 virions do not bind blood coagulation factor X and cause low random transduction upon vascular delivery; (2) they clear host tissues more quickly than do traditionally used Ad5 vectors; (3) Ad43 uses CD46 as primary receptor; (4) Ad43 can use integrins as alternative primary receptors. As the first step toward vectorization of Ad43, we demonstrated that the primary receptor specificity of the Ad43 fiber can be altered to achieve infection via Her2, an established oncotarget. Whereas this modification required use of the Ad5 fiber shaft, the presence of this domain in chimeric virions did not make them susceptible for neutralization by anti-Ad5 antibodies.

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Native and engineered tropism of vectors derived from a rare species D adenovirus serotype 43

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

Access to Document

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