Literature DB >> 17014674

Strategies to enhance transductional efficiency of adenoviral-based gene transfer to primary human fibroblasts and keratinocytes as a platform in dermal wounds.

Alexander Stoff1, Angel A Rivera, N S Banerjee, J Michael Mathis, Antonio Espinosa-de-los-Monteros, Long P Le, Jorge I De la Torre, Luis O Vasconez, Thomas R Broker, Dirk F Richter, Mariam A Stoff-Khalili, David T Curiel.   

Abstract

Genetically modified keratinocytes and fibroblasts are suitable for delivery of therapeutic genes capable of modifying the wound healing process. However, efficient gene delivery is a prerequisite for successful gene therapy of wounds. Whereas adenoviral vectors (Ads) exhibit superior levels of in vivo gene transfer, their transductional efficiency to cells resident within wounds may nonetheless be suboptimal, due to deficiency of the primary adenovirus receptor, coxsackie-adenovirus receptor (CAR). We explored CAR-independent transduction to fibroblasts and keratinocytes using a panel of CAR-independent fiber-modified Ads to determine enhancement of infectivity. These fiber-modified adenoviral vectors included Ad 3 knob (Ad5/3), canine Ad serotype 2 knob (Ad5CAV-2), RGD (Ad5.RGD), polylysine (Ad5.pK7), or both RGD and polylysine (Ad5.RGD.pK7). To evaluate whether transduction efficiencies of the fiber-modified adenoviral vectors correlated with the expression of their putative receptors on keratinocytes and fibroblasts, we analyzed the mRNA levels of CAR, alpha upsilon integrin, syndecan-1, and glypican-1 using quantitative polymerase chain reaction. Analysis of luciferase and green fluorescent protein transgene expression showed superior transduction efficiency of Ad5.pK7 in keratinocytes and Ad5.RGD.pK7 in fibroblasts. mRNA expression of alpha upsilon integrin, syndecan-1 and glypican-1 was significantly higher in primary fibroblasts than CAR. In keratinocytes, syndecan-1 expression was significantly higher than all the other receptors tested. Significant infectivity enhancement was achieved in keratinocytes and fibroblasts using fiber-modified adenoviral vectors. These strategies to enhance infectivity may help to achieve higher clinical efficacy of wound gene therapy.

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Year:  2006        PMID: 17014674      PMCID: PMC2203209          DOI: 10.1111/j.1743-6109.2006.00168.x

Source DB:  PubMed          Journal:  Wound Repair Regen        ISSN: 1067-1927            Impact factor:   3.617


  46 in total

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5.  Gene transfer to cervical cancer with fiber-modified adenoviruses.

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Authors:  Sundeep G Keswani; Anna B Katz; Foong-Yen Lim; Philip Zoltick; Antoneta Radu; Datis Alaee; Meenhard Herlyn; Timothy M Crombleholme
Journal:  Wound Repair Regen       Date:  2004 Sep-Oct       Impact factor: 3.617

9.  Preclinical evaluation of a class of infectivity-enhanced adenoviral vectors in ovarian cancer gene therapy.

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2.  The noninvasive, quantitative, in vivo assessment of adenoviral-mediated gene delivery in skin wound biomaterials.

Authors:  Carrie Y Peterson; Ashkaun Shaterian; Alexandra K Borboa; Ana M Gonzalez; Bruce M Potenza; Raul Coimbra; Brian P Eliceiri; Andrew Baird
Journal:  Biomaterials       Date:  2009-09-24       Impact factor: 12.479

3.  Selective transduction of mature DC in human skin and lymph nodes by CD80/CD86-targeted fiber-modified adenovirus-5/3.

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Journal:  J Immunother       Date:  2009 Nov-Dec       Impact factor: 4.456

4.  Enhanced Delivery of Oncolytic Adenovirus by Neural Stem Cells for Treatment of Metastatic Ovarian Cancer.

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  4 in total

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