An adenovirus vector with a chimeric fiber incorporating stabilized single chain antibody achieves targeted gene delivery

Hedley, Susan J.; Maur, Adrian Auf der; Hohn, S.; Escher, Dominik; Barberis, Alcide; Glasgow, Joel N.; Douglas, Joanne T.; Korokhov, Nikolay; Curiel, David T.

doi:10.1038/sj.gt.3302603

Cited by 60 publications

(53 citation statements)

References 42 publications

(46 reference statements)

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“…Vector attachment to FRa was redirected, but gene delivery was not achieved (47). Display of scFvs on adenoviruses remains challenging as the folding of scFv occurs in the endoplasmic reticulum, whereas adenoviral assembly does not (48,49).…”

Section: Discussionmentioning

confidence: 99%

The Use of a Tropism-Modified Measles Virus in Folate Receptor–Targeted Virotherapy of Ovarian Cancer

Hasegawa¹,

Nakamura²,

Harvey³

et al. 2006

Clinical Cancer Research

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Purpose: Attenuated measles viruses are promising experimental anticancer agents currently being evaluated in a phase I dose escalation trial for ovarian cancer patients. Virus attachment, entry, and subsequent intercellular fusion between infected and uninfected neighboring cells are mediated via the two measles receptors (CD46 and SLAM). To minimize potential toxicity due to measles virus–associated immunosuppression and infection of nontarget tissues, we sought to develop an ovarian cancer exclusive fully retargeted measles virus. Experimental Design and Results: Interactions of measles virus with its natural receptors were ablated, and a single-chain antibody (scFv) specific for α-folate receptor (FRα), a target overexpressed on 90% of nonmucinous ovarian cancer, was genetically engineered on the viral attachment protein (MV-αFR). Specificity of virus tropism was tested on tumor and normal cells. Biodistribution of measles virus infection was evaluated in measles-susceptible CD46 transgenic mice, whereas antitumor activity was monitored noninvasively by bioluminescence imaging in xenograft models. Tropism and fusogenic activity of MV-αFR was redirected exclusively to FRα without compromise to virus infectivity. In contrast to the parental virus, MV-αFR has no background infectivity on normal human cells. The antitumor activity of MV-αFR, as assessed by tumor volume reduction and overall survival increase, was equal to the parental virus in two models of human ovarian cancer (s.c. and i.p.). Conclusions: A FR-exclusive ovarian cancer targeted oncolytic virus was generated and shown to be therapeutically effective, thus introducing a new modality for FR targeting and a candidate measles virus for clinical testing.

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Section: Discussionmentioning

confidence: 99%

The Use of a Tropism-Modified Measles Virus in Folate Receptor–Targeted Virotherapy of Ovarian Cancer

Hasegawa¹,

Nakamura²,

Harvey³

et al. 2006

Clinical Cancer Research

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show abstract

“…117 On this basis, rational development of complex ligands with cytoplasmic solubility and stability will be required for their application to Ad vectors. Exemplifying this concept, Hedley et al 118 have developed a singlecomponent antibody-targeted Ad vector by incorporating a novel, cytoplasmically stable scFv into a de-knobbed fiber. This vector demonstrated selective targeting to its cognate epitope expressed on the membrane surface of cells, and suggests that cytoplasmic stability of the targeting molecule, per se, allows retention of antigen recognition in the Ad capsid-incorporated context.…”

Section: Adenovirus Targeting Via Genetic Modification: Fibermentioning

confidence: 99%

Transductional targeting of adenovirus vectors for gene therapy

2006

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“…The stock virus was then used to infect HEK293 cells for the preparation of fiber-modified Ad. The viruses were purified on CsCl and dialyzed against Tris-buffered saline (20 mM Tris-HCl, pH 8.1) as previously described (19). The titers of the purified viruses were determined by measuring protein content using bovine serum albumin as a standard.…”

Section: Construction Of 9r Fste-modified Adenoviral Vectorsmentioning

confidence: 99%

“…It was found that the fiber knob at the C terminus, but not the N-terminal half (1 to 260 aa), was required for fiber trimer formation (23) since fiber proteins containing the knob and two or more shaft repeats form functional trimers. Those find-ings have since been used to guide fiber modification for improved gene delivery, including peptide insertion at the knob region or peptide fusion at the fiber C terminus (11,19,21,27,28,35). In most cases, the modified viruses retain the native tropism while regaining some specificity associated with the inserted oligopeptides.…”

mentioning

confidence: 99%

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Adenovirus Fiber Shaft Contains a Trimerization Element That Supports Peptide Fusion for Targeted Gene Delivery

Lad

Yang

et al. 2006

J Virol

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Adenoviral (Ad) vectors have been widely used in human gene therapy clinical trials. However, their application has frequently been restricted by the unfavorable expression of cell surface receptors critical for Ad infection. Infections by Ad2 and Ad5 are largely regulated by the elongated fiber protein that mediates its attachment to a cell surface receptor, coxsackie and adenovirus receptor (CAR). The fiber protein is a homotrimer consisting of an N-terminal tail, a long shaft, and a C-terminal knob region that is responsible for high-affinity receptor binding and Ad tropism. Consequently, the modification of the knob region, including peptide insertion and C-terminal fusion of ligands for cell surface receptors, has become a major research focus for targeting gene delivery. Such manipulation tends to disrupt fiber assembly since the knob region contains a stabilization element for fiber trimerization. We report here the identification of a novel trimerization element in the Ad fiber shaft. We demonstrate that fiber fragments containing the N-terminal tail and shaft repeats formed stable trimers that assembled onto Ad virions independently of the knob region. This fiber shaft trimerization element (FSTE) exhibited a capacity to support peptide fusion. We showed that Ad, modified with a chimeric protein by direct fusion of the FSTE with a growth factor ligand or a single-chain antibody, delivered a reporter gene selectively. Together, these results indicate that the shaft region of Ad fiber protein contains a trimerization element that allows ligand fusion, which potentially broadens the basis for Ad vector development.

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An adenovirus vector with a chimeric fiber incorporating stabilized single chain antibody achieves targeted gene delivery

Cited by 60 publications

References 42 publications

The Use of a Tropism-Modified Measles Virus in Folate Receptor–Targeted Virotherapy of Ovarian Cancer

The Use of a Tropism-Modified Measles Virus in Folate Receptor–Targeted Virotherapy of Ovarian Cancer

Transductional targeting of adenovirus vectors for gene therapy

Adenovirus Fiber Shaft Contains a Trimerization Element That Supports Peptide Fusion for Targeted Gene Delivery

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