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腺病毒5型六邻体介导肝脏基因转移。

Adenovirus serotype 5 hexon mediates liver gene transfer.

作者信息

Waddington Simon N, McVey John H, Bhella David, Parker Alan L, Barker Kristeen, Atoda Hideko, Pink Rebecca, Buckley Suzanne M K, Greig Jenny A, Denby Laura, Custers Jerome, Morita Takashi, Francischetti Ivo M B, Monteiro Robson Q, Barouch Dan H, van Rooijen Nico, Napoli Claudio, Havenga Menzo J E, Nicklin Stuart A, Baker Andrew H

机构信息

Department of Haematology, Haemophilia Centre and Haemostasis Unit, Royal Free and University College Medical School, London NW3 2PF, UK.

出版信息

Cell. 2008 Feb 8;132(3):397-409. doi: 10.1016/j.cell.2008.01.016.


DOI:10.1016/j.cell.2008.01.016
PMID:18267072
Abstract

Adenoviruses are used extensively as gene transfer agents, both experimentally and clinically. However, targeting of liver cells by adenoviruses compromises their potential efficacy. In cell culture, the adenovirus serotype 5 fiber protein engages the coxsackievirus and adenovirus receptor (CAR) to bind cells. Paradoxically, following intravascular delivery, CAR is not used for liver transduction, implicating alternate pathways. Recently, we demonstrated that coagulation factor (F)X directly binds adenovirus leading to liver infection. Here, we show that FX binds to the Ad5 hexon, not fiber, via an interaction between the FX Gla domain and hypervariable regions of the hexon surface. Binding occurs in multiple human adenovirus serotypes. Liver infection by the FX-Ad5 complex is mediated through a heparin-binding exosite in the FX serine protease domain. This study reveals an unanticipated function for hexon in mediating liver gene transfer in vivo.

摘要

腺病毒在实验和临床中都被广泛用作基因传递载体。然而,腺病毒对肝细胞的靶向作用会影响其潜在疗效。在细胞培养中,腺病毒血清型5纤维蛋白与柯萨奇病毒和腺病毒受体(CAR)结合以附着细胞。矛盾的是,在血管内递送后,CAR并不用于肝脏转导,这意味着存在其他途径。最近,我们证明凝血因子(F)X直接结合腺病毒导致肝脏感染。在此,我们表明FX通过FX Gla结构域与六邻体表面高变区之间的相互作用,与Ad5六邻体而非纤维结合。这种结合在多种人类腺病毒血清型中都存在。FX-Ad5复合物对肝脏的感染是通过FX丝氨酸蛋白酶结构域中的一个肝素结合外部位点介导的。这项研究揭示了六邻体在介导体内肝脏基因转移方面的一种意想不到的功能。

相似文献

[1]
Adenovirus serotype 5 hexon mediates liver gene transfer.

Cell. 2008-2-8

[2]
Substitution of adenovirus serotype 3 hexon onto a serotype 5 oncolytic adenovirus reduces factor X binding, decreases liver tropism, and improves antitumor efficacy.

Mol Cancer Ther. 2010-8-24

[3]
Identification of coagulation factor (F)X binding sites on the adenovirus serotype 5 hexon: effect of mutagenesis on FX interactions and gene transfer.

Blood. 2009-7-30

[4]
Cell entry and trafficking of human adenovirus bound to blood factor X is determined by the fiber serotype and not hexon:heparan sulfate interaction.

PLoS One. 2011-5-26

[5]
Adenovirus serotype 5 hexon is critical for virus infection of hepatocytes in vivo.

Proc Natl Acad Sci U S A. 2008-4-8

[6]
Human full-length coagulation factor X and a GLA domain-derived 40-mer polypeptide bind to different regions of the adenovirus serotype 5 hexon capsomer.

Hum Gene Ther. 2014-4

[7]
Biodistribution and retargeting of FX-binding ablated adenovirus serotype 5 vectors.

Blood. 2010-7-7

[8]
Biodistribution and inflammatory profiles of novel penton and hexon double-mutant serotype 5 adenoviruses.

J Control Release. 2012-5-22

[9]
Requirements for receptor engagement during infection by adenovirus complexed with blood coagulation factor X.

PLoS Pathog. 2010-10-7

[10]
Coagulation factor binding orientation and dimerization may influence infectivity of adenovirus-coagulation factor complexes.

J Virol. 2013-6-26

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