Journal ArticleDOI
Glutathione-sensitive RGD-poly(ethylene glycol)-SS-polyethylenimine for intracranial glioblastoma targeted gene delivery.
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TLDR
The present study aimed to enhance the low transfection efficiency caused by PEGylation by taking advantage of a nonviral vector containing a disulfide linkage.Abstract:
Background
Reductively reversible and hydrolytically degradable cationic polymers have been used as gene delivery systems. The present study aimed to enhance the low transfection efficiency caused by PEGylation by taking advantage of a nonviral vector containing a disulfide linkage.
Methods
The novel reducible targeted gene vector c(RGDyK)-poly(ethylene glycol)-SS-polyethylenimine (RGD-PEG-SS-PEI), representing a combination of RGD-PEG with PEI through a disulfide linkage, was synthesized and its reduction-sensitivity was tested in the presence of glutathione. The RGD-PEG-SS-PEI/pDNA complexes were formed and their stability was evaluated by agarose gel electrophoresis in both phosphate-buffered saline and Dulbecco's modified Eagle's medium with 10% serum. In vitro transfection efficiency and cell viability assay of the different polymers was performed for U87 cells using pEGFP-N2 and pGL4.2 reporter gene systems. RGD-PEG-SS-PEI/pDsRED-N1 and RGD-PEG-PEI/pDsRED-N1 complexes were injected intravenously into the U87 cell-bearing nude mice via their tail vein to investigate in vivo gene expression.
Results
RGD-PEG-SS-PEI has been synthesized successfully and its reduction-sensitivity was confirmed in the presence of glutathione. The RGD-PEG-SS-PEI/pDNA complexes demonstrated good stability in both conditions. In comparison with mPEG-PEI/pDNA for gene delivery, the RGD-PEG-SS-PEI/pDNA complex provided improved levels of transfection efficiency and reduced cytotoxicity when tested in U87 cells in vitro, and also enhanced levels of gene expression in the brains of intracranial U87 glioblastoma-bearing mice as demonstrated using dsRed gene transfer and bioimaging in vivo.
Conclusions
The results of the present study suggest that RGD-PEG-SS-PEI represents a promising candidate for further study in glioblastoma and combined gene therapies. Copyright © 2013 John Wiley & Sons, Ltd.read more
Citations
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Internal stimuli-responsive nanocarriers for drug delivery: Design strategies and applications.
TL;DR: Current functional moieties responsive to a variety of internal stimuli, including pH, redox, enzyme, temperature are presented and can provide inspiration and impetus for exploiting more promising internal stimuli-responsive nano-systems for drug delivery.
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In vivo gene delivery mediated by non-viral vectors for cancer therapy.
Reza Mohammadinejad,Ali Dehshahri,Vijay Sagar Madamsetty,Masoumeh Zahmatkeshan,Shima Tavakol,Pooyan Makvandi,Danial Khorsandi,Abbas Pardakhty,Milad Ashrafizadeh,Elham Ghasemipour Afshar,Ali Zarrabi +10 more
TL;DR: The in vivo gene delivery mediated by non-viral vectors to treat cancer in different tissue and organs including brain, breast, lung, liver, stomach, and prostate is highlighted and the state-of-the-art and promising perspective of in vitro gene editing using non-Viral nano-vectors is delineated.
Journal ArticleDOI
Major degradable polycations as carriers for DNA and siRNA
Mohammad Ariful Islam,Tae-Eun Park,Bijay Singh,Sushila Maharjan,Jannatul Firdous,Myung-Haing Cho,Sang-Kee Kang,Cheol-Heui Yun,Yun-Jaie Choi,Chong-Su Cho +9 more
TL;DR: The recent developments on these three major degradable polycations as promising carriers for deoxyribonucleic acid (DNA) and small interfering RNA (siRNA) are explained.
Journal ArticleDOI
Biodegradable Polymers for Gene-Delivery Applications
TL;DR: The aim of this review is to introduce the recent development and progress of biodegradable polymers for gene delivery applications, especially for their chemical structure design, gene delivery capacity and additional biological functions.
Journal ArticleDOI
Vectors for Glioblastoma Gene Therapy: Viral & Non-Viral Delivery Strategies
TL;DR: Delivery systems including viral, non-polymeric, and polymeric vectors that have been used in glioblastoma multiforme (GBM) gene therapy are discussed.
References
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Journal ArticleDOI
A versatile vector for gene and oligonucleotide transfer into cells in culture and in vivo: polyethylenimine
Otmane Boussif,Frank Lezoualc'h,Maria Antonietta Zanta,Mojgan Mergny,Daniel Scherman,Barbara A. Demeneix,Jean-Paul Behr +6 more
TL;DR: Together, these properties make PEI a promising vector for gene therapy and an outstanding core for the design of more sophisticated devices because its efficiency relies on extensive lysosome buffering that protects DNA from nuclease degradation, and consequent lysOSomal swelling and rupture that provide an escape mechanism for the PEI/DNA particles.
Journal ArticleDOI
Redox environment of the cell as viewed through the redox state of the glutathione disulfide/glutathione couple.
TL;DR: Estimates can be used to more fully understand the redox biochemistry that results from oxidative stress, which hopefully will provide a rationale and understanding of the cellular mechanisms associated with cell growth and development, signaling, and reductive or oxidative stress.
Journal ArticleDOI
PEGylation, successful approach to drug delivery.
TL;DR: Polyethylene glycol-drug conjugates have several advantages: a prolonged residence in body, a decreased degradation by metabolic enzymes and a reduction or elimination of protein immunogenicity.
Journal ArticleDOI
Drug delivery strategy utilizing conjugation via reversible disulfide linkages: role and site of cellular reducing activities
TL;DR: This review focuses on understanding where and how the disulfide bond in the bioconjugate is reduced upon contact with biological milieu, which affects delivery design and the interpretation of the delivery strategies.
Journal ArticleDOI
PEGylated DNA/transferrin–PEI complexes: reduced interaction with blood components, extended circulation in blood and potential for systemic gene delivery
TL;DR: In tumor bearing mice, application of non-PEGylated complexes through the tail vein resulted in reporter gene expression in tail and lung, but severe toxicity was observed in some mice, while PEGylation of the complexes mediated reporter gene transfer to the tumor without significant toxicity.