Literature DB >> 17019592

Gene delivery by cationic lipid vectors: overcoming cellular barriers.

Inge S Zuhorn1, Jan B F N Engberts, Dick Hoekstra.   

Abstract

Non-viral vectors such as cationic lipids are capable of delivering nucleic acids, including genes, siRNA or antisense RNA into cells, thus potentially resulting in their functional expression. These vectors are considered as an attractive alternative for virus-based delivery systems, which may suffer from immunological and mutational hazards. However, the efficiency of cationic-mediated gene delivery, although often sufficient for cell biological purposes, runs seriously short from a therapeutics point of view, as realizing this objective requires a higher level of transfection than attained thus far. To develop strategies for improvement, there is not so much a need for novel delivery systems. Rather, better insight is needed into the mechanism of delivery, including lipoplex-cell surface interaction, route of internalization and concomitant escape of DNA/RNA into the cytosol, and transport into the nucleus. Current work indicates that a major obstacle involves the relative inefficient destabilization of membrane-bounded compartments in which lipoplexes reside after their internalization by the cell. Such an activity requires the capacity of lipoplexes of undergoing polymorphic transitions such as a membrane destabilizing hexagonal phase, while cellular components may aid in this process. A consequence of the latter notion is that for development of a novel generation of delivery devices, entry pathways have to be triggered by specific targeting to select delivery into intracellular compartments which are most susceptible to lipoplex-induced destabilization, thereby allowing the most efficient release of DNA, a minimal requirement for optimizing non-viral vector-mediated transfection.

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Year:  2006        PMID: 17019592     DOI: 10.1007/s00249-006-0092-4

Source DB:  PubMed          Journal:  Eur Biophys J        ISSN: 0175-7571            Impact factor:   2.095


  98 in total

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2.  Transfection mediated by pH-sensitive sugar-based gemini surfactants; potential for in vivo gene therapy applications.

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3.  Determining the size and shape dependence of gold nanoparticle uptake into mammalian cells.

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4.  PS exposure increases the susceptibility of cells to fusion with DOTAP liposomes.

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Journal:  Chem Biol Interact       Date:  2006-02-17       Impact factor: 5.192

5.  Effects of divalent cations and pH on phosphatidylserine model membranes: a 31P NMR study.

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6.  Extraction of cholesterol with methyl-beta-cyclodextrin perturbs formation of clathrin-coated endocytic vesicles.

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Review 7.  Barriers to carrier mediated drug and gene delivery to brain tumors.

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8.  Phase behavior of cationic amphiphiles and their mixtures with helper lipid influences lipoplex shape, DNA translocation, and transfection efficiency.

Authors:  Inge S Zuhorn; Volker Oberle; Willy H Visser; Jan B F N Engberts; Udo Bakowsky; Evgeny Polushkin; Dick Hoekstra
Journal:  Biophys J       Date:  2002-10       Impact factor: 4.033

9.  Transferrin-modified liposomes equipped with a pH-sensitive fusogenic peptide: an artificial viral-like delivery system.

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10.  Antisense oligonucleotides reach mRNA targets via the RNA matrix: downregulation of the 5-HT1A receptor.

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  45 in total

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Review 6.  Current status of non-viral gene therapy for CNS disorders.

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7.  Cationic lipid nanodisks as an siRNA delivery vehicle.

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8.  Characterization of liposomes for cancer cell transfection.

Authors:  Svetlana A Tatarkova; Satvinder Khaira
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9.  Design of hybrid lipid/retroviral-like particle gene delivery vectors.

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10.  Very long chain N4, N9 -diacyl spermines: non-viral lipopolyamine vectors for efficient plasmid DNA and siRNA delivery.

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