A novel conditionally replicating adenoviral vector with dual expression of IL-24 and arresten inserted in E1 and the region between E4 and fiber for improved melanoma therapy

Chai, Lihong; Liu, S; Mao, Qinwen; Wang, D; Li, X; Zheng, Xiaojing; Xia, Haibin

doi:10.1038/cgt.2011.84

Cited by 21 publications

(12 citation statements)

References 33 publications

(35 reference statements)

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“…A couple of studies have also shown that a CRAd carrying IL-24 helped in inducing apoptosis of melanoma cells following radiotherapy (Chai et al , 2012; Jiang et al , 2012). Thus, the possibility of acting on human melanoma tumors with an oncolytic virus that can target both the stromal and the malignant compartment, respond to melanoma microenvironment, and whose infectivity can be tailored according to cell surface expression of viral receptors can be of significant importance for melanoma therapeutics.…”

Section: Discussionmentioning

confidence: 99%

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Viale

Cafferata

Gould

et al. 2013

Journal of Investigative Dermatology

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We have previously designed a conditionally replicative oncolytic adenovirus (CRAd) named Ad-F512 that can target both the stromal and the malignant melanoma cell compartments. The replication capacity of this CRAd is driven by a 0.5-Kb SPARC promoter fragment (named F512). To improve CRAd’s efficacy, we cloned into F512 motives responsive to hypoxia (hypoxia-responsive element (HRE)) and inflammation (nuclear factor kappa B) to obtain a chimeric promoter named κBF512HRE. Using luciferase as a reporter gene, we observed 10–15-fold increased activity under hypoxia and 10–80-fold induction upon tumor necrosis factor-α addition. We next constructed a CRAd (Ad-κBF512HRE) where E1A activity was under κBF512HRE regulation. Treatment of nude mice harboring established tumors made of a mix of SB2 melanoma cells and WI-38 fibroblasts with Ad-κBF512HRE led to the complete elimination of tumors in 100% of mice (8/8). Moreover, Ad-5/3-κBF512HRE, a viral variant pseudotyped with a chimeric 5/3 fiber, exerted a strong lytic effect on CAR-negative melanoma cells and was highly effective in vivo on established tumors made of melanoma cells and WI-38 fibroblasts, leading to the complete elimination of 4/5 tumors. These results indicate that this improved stroma-targeted oncolytic adenovirus can override the resistance of melanoma tumors and might become of significant importance for melanoma therapeutics.

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Section: Discussionmentioning

confidence: 99%

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Viale

Cafferata

Gould

et al. 2013

Journal of Investigative Dermatology

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“…Adenoviruses have several advantages over some other viral vectors such as retroviruses and adeno-associated virus. Adenovirus vectors can infect a variety of cell types, including non-dividing as well as dividing cells, and can be prepared readily in large quantities in tissue culture (Vetrini and Ng, 2010;Chai et al, 2012) 1.4.1.5 Adenovirus-based vaccines against infectious pathogens Another promising application for adenoviruses is their use as vaccine vectors (Gaydos and Gaydos, 1995). As already mentioned, live, oral, enteric-coated, adenovirus serotypes 4 and 7 vaccines were safely used for years in military training camps to prevent epidemics of acute adenoviral respiratory disease.…”

Section: The Use Of Adenovirus Vectors For Gene Therapymentioning

confidence: 99%

Adenoviruses

Allard¹,

Vantarakis²

2019

Water and Sanitation for the 21st Century: Health and Microbiological Aspects of Excreta and Wastewater Management (Global Wate

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The designations employed and the presentation of material throughout this publication do not imply the expression of any opinion whatsoever on the part of UNESCO concerning the legal status of any country, territory, city or area or of its authorities, or concerning the delimitation of its frontiers or boundaries. The ideas and opinions expressed in this publication are those of the authors; they are not necessarily those of UNESCO and do not commit the Organization.

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“…Early versions of dualexpression vectors carried two versions of the same cassette within E1 that differed in the transgene but contained the identical (Zinn et al, 2002) or different (Liu et al, 2012) regulatory elements. Others used bidirectional promoters to control up-and downstream transgenes placed into E1 (Chai et al, 2011) or two expression cassettes with different promoters placed in tandem into E1 (Irie et al, 2005). Others, similar to our approach, inserted one transgene under the control of a CMV promoter into E1 and a second transgene under the control of the RSV promoter into E3 with both expression cassettes in the same orientation (Niu et al, 2006).…”

Section: Dual-expression Adenoviral Vectorsmentioning

confidence: 99%

Construction and Characterization of E1- and E3-Deleted Adenovirus Vectors Expressing Two Antigens from Two Separate Expression Cassettes

Small

Kurupati²,

Zhou³

et al. 2014

Human Gene Therapy

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Here we describe a series of replication-defective adenovirus vectors designed to express transgene products from two expression cassettes placed into the deleted E1 and E3 domains. Vectors that contained an E1 cassette with a cytomegalovirus promoter in the forward orientation and an E3 cassette with the chicken β-actin promoter in the reverse orientation grew to acceptable yields and expressed both transgenes. Additionally, they elicited immune responses to both transgene products. Levels of expression and the vectors' immunogenicity were influenced by the presence of regulatory elements shared between the two expression cassettes. Specifically, vectors that carried the same intron and enhancer in both expression cassettes could be rescued and expanded, but they were poorly immunogenic. Deletion of the enhancer or both the enhancer and the intron from the E3 cassette increased T- and B-cell responses to both transgene products.

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A novel conditionally replicating adenoviral vector with dual expression of IL-24 and arresten inserted in E1 and the region between E4 and fiber for improved melanoma therapy

Cited by 21 publications

References 33 publications

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Therapeutic Improvement of a Stroma-Targeted CRAd by Incorporating Motives Responsive to the Melanoma Microenvironment

Adenoviruses

Construction and Characterization of E1- and E3-Deleted Adenovirus Vectors Expressing Two Antigens from Two Separate Expression Cassettes

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