Literature DB >> 24370892

Polymer-enhanced delivery increases adenoviral gene expression in an orthotopic model of bladder cancer.

Helen Gosnell1, Laura M Kasman1, Thrimoorthy Potta2, Lucas Vu2, Elizabeth Garrett-Mayer3, Kaushal Rege2, Christina Voelkel-Johnson4.   

Abstract

Gene therapy has garnered significant attention as a therapeutic approach for bladder cancer but efficient delivery and gene expression remain major hurdles. The goal of this study was to determine if cationic polymers can enhance adenoviral gene expression in cells that are difficult to transduce in vitro and to subsequently investigate lead candidates for their capacity to increase adenoviral gene expression in an orthotopic in vivo model of bladder cancer. In vitro screening of linear polyamine-based and aminoglycoside-based polymer libraries identified several candidates that enhanced adenoviral reporter gene expression in vitro. The polyamine-based polymer NPGDE-1,4 Bis significantly enhanced adenoviral gene expression in the orthotopic model of bladder cancer but unfortunately further use of this polymer was limited by toxicity. In contrast, the aminoglycoside-based polymer paromomycin-BGDE, enhanced adenoviral gene expression within the bladder without adverse events. Our study demonstrates for the first time that cationic polymers can enhance adenoviral gene expression in an orthotopic model of bladder cancer, thereby providing the foundation for future studies to determine therapeutic benefits of polymer-adenovirus combination in bladder cancer gene therapy.
Copyright © 2013 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Adenovirus; Bladder cancer; Cationic polymer; Gene delivery; Orthotopic

Mesh:

Substances:

Year:  2013        PMID: 24370892      PMCID: PMC3952388          DOI: 10.1016/j.jconrel.2013.12.012

Source DB:  PubMed          Journal:  J Control Release        ISSN: 0168-3659            Impact factor:   9.776


  37 in total

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2.  AdCD40L immunogene therapy for bladder carcinoma--the first phase I/IIa trial.

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Review 4.  Discovery of cationic polymers for non-viral gene delivery using combinatorial approaches.

Authors:  Sutapa Barua; James Ramos; Thrimoorthy Potta; David Taylor; Huang-Chiao Huang; Gabriela Montanez; Kaushal Rege
Journal:  Comb Chem High Throughput Screen       Date:  2011-12       Impact factor: 1.339

5.  An orthotopic bladder cancer model for gene delivery studies.

Authors:  Laura Kasman; Christina Voelkel-Johnson
Journal:  J Vis Exp       Date:  2013-12-01       Impact factor: 1.355

6.  The effect of surface modification of adenovirus with an arginine-grafted bioreducible polymer on transduction efficiency and immunogenicity in cancer gene therapy.

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7.  Local AdCD40L gene therapy is effective for disseminated murine experimental cancer by breaking T-cell tolerance and inducing tumor cell growth inhibition.

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8.  Polymer-enhanced adenoviral transduction of CAR-negative bladder cancer cells.

Authors:  Laura M Kasman; Sutapa Barua; Ping Lu; Kaushal Rege; Christina Voelkel-Johnson
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Review 9.  Progress in developing cationic vectors for non-viral systemic gene therapy against cancer.

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  9 in total

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4.  Electrostatic interaction of tumor-targeting adenoviruses with aminoclay acquires enhanced infectivity to tumor cells inside the bladder and has better cytotoxic activity.

Authors:  Soo-Yeon Kim; Whi-An Kwon; Seung-Pil Shin; Ho Kyung Seo; Soo-Jeong Lim; Yuh-Seog Jung; Hyo-Kyung Han; Kyung-Chae Jeong; Sang-Jin Lee
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5.  Folate receptor-targeted aminoglycoside-derived polymers for transgene expression in cancer cells.

Authors:  Sudhakar Godeshala; Rajeshwar Nitiyanandan; Brian Thompson; Sheba Goklany; David R Nielsen; Kaushal Rege
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6.  Gold nanoparticle coatings as efficient adenovirus carriers to non-infectable stem cells.

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7.  Bioreducible Poly(Amino Ethers) Based mTOR siRNA Delivery for Lung Cancer.

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8.  A Biomimic Reconstituted High-Density-Lipoprotein-Based Drug and p53 Gene Co-delivery System for Effective Antiangiogenesis Therapy of Bladder Cancer.

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9.  Parallel synthesis of poly(amino ether)-templated plasmonic nanoparticles for transgene delivery.

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  9 in total

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