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51. Gene delivery to the lung using protein/polyethylenimine/plasmid complexes.

Author

Orson, F.M., Song, L., Gautam, A., Densmore, C.L., Bhogal, B.S., and Kinsey, B.M.

Subjects
GENE therapy, LUNGS, PLASMIDS
Abstract

Delivery of genes to the lung has enormous potential in a wide variety of illnesses, from lung cancer to genetic deficiency diseases. Many delivery systems have been utilized, each with its own advantages and limitations. Polyethylenimine is a polycation capable of binding and compacting DNA, enabling intravascular plasmid delivery to normal tissues in such a way that the plasmid can be expressed in a proportion of the exposed cells. We have developed a novel intravenous method to deliver small amounts of plasmid to lung tissue, using nontoxic quantities of polyethylenimine in combination with albumin (or other soluble proteins). Injection of 1 µg or less of plasmid resulted in highly efficient gene expression in lung interstitial and endothelial tissues (0.5 to 1 ng luciferase per µg plasmid DNA), while larger quantities of plasmid reduced relative gene expression. Using luciferase as a reporter gene, single injections had maximal gene expression between 24 and 48 h, with a rapid decline thereafter, in contrast to some other delivery systems, however, no inhibition of gene expression occurred during multiple rounds of plasmid administration through 20 days. As a result, this method may have useful applications in diseases that could benefit from recurrent therapeutic gene delivery. [ABSTRACT FROM AUTHOR]

Published
2002
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52. Author Index.

Subjects
AUTHORS, GENE therapy
Abstract

Lists contributing authors to the December 2001 issue of the periodical 'Gene Therapy.' M.C. Aalders; A. Adler; R.R. Ali; A. Balmain; Q. Chen; T. Daemen.

Published
2001
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53. Structure of transfection-active histone H1/DNA complexes.

Author

Lucius, Hans, Haberland, Annekathrin, Zaitsev, Sergei, Dallüge, Roman, Schneider, Marc, and Böttger, Michael

Abstract

Relationships between the structure of transfecting complexes of histone H1 and DNA and their transfection efficiency were studied. Transfection activity proved to be connected to complex aggregates. Low speed centrifugation of the complexes resulted in loss of the transfection activity. The complexes/aggregates were active with high efficiency in a broad range of weight input ratios ri (0.1< ri<30). Using atomic force microscopy (AFM), the complexes were imaged at negative, nearly electroneutral and positive charge conditions. Electroneutral complexes at ri=1 showed a multitude of different complex forms. Fibrillar, network-like and branched structures were frequently present in one complex. Strongly positive charged complexes had a toroidal appearance. All these different forms contributed to the high transfection efficiency. Cellular uptake is supposed to be by phagocytosis. [ABSTRACT FROM AUTHOR]

Published
2001
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55. Polyethylenimine/DNA complexes shielded by transferrin target gene expression to tumors after systemic application.

Author

Kircheis, R, Wightman, L, Schreiber, A, Robitza, B, Rössler, V, Kursa, M, and Wagner, E

Subjects
POLYMERS, DNA, TRANSFERRIN, GENETIC transformation
Abstract

Systemic application of positively charged polycation/DNA complexes has been shown to result in predominant gene expression in the lungs. Targeting gene expression to other sites, eg distant tumors, is hampered by nonspecific interactions largely due to the positive surface charge of transfection complexes. In the present study we show that the positive surface charge of PEI (25 kDa branched or 22 kDa linear)/DNA complexes can be efficiently shielded by covalently incorporating transferrin at sufficiently high densities in the complex, resulting in a dramatic decrease in nonspecific interactions, eg with erythrocytes, and decreased gene expression in the lung. Systemic application of transferrinshielded PEI/DNA complexes into A/J mice bearing subcutaneously growing Neuro2a tumors via the taft vein resulted in preferential (100- to 500-fold higher) luciferase reporter gene expression in distant tumors as compared with the major organs including the lungs. Tumor targeting is also demonstrated by DNA uptake and β-galactosidase gene expression in tumor cells. Assessing DNA distribution following systemic application significant amounts of DNA were found in the liver and tumor. However, in the liver, DNA was mainly taken up by Kupffer cells and degraded without significant transgene expression. In the tumor, DNA was associated mainly with tumor cells and frequently found near structures which resemble primitive blood vessels. [ABSTRACT FROM AUTHOR]

Published
2001
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56. Author Index.

Subjects
AUTHORS, GENE therapy
Abstract

Presents an index to authors of articles in volume 7, 2000, of the journal 'Gene Therapy.'

Published
2000
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57. Ovarian carcinoma cells are effectively transfected by polyethylenimine (PEI) derivatives.

Author

Poulain, Laurent, Ziller, Christelle, Muller, Christian D, Erbacher, Patrick, Bettinger, Thierry, Rodier, Jean-François, and Behr, Jean-Paul

Subjects
OVARIAN diseases, GENETIC transformation, CELL lines, GENETICS
Abstract

As a prerequisite to nonviral gene therapy approaches of ovarian carcinoma, we evaluated the possibility of transfecting established tumor cell lines (SKOV3, IGROV1) as well as primary mesothelial and tumor cells by various polyethylenimine (PEI) derivatives. Several PEI-based vectors were able to effectively transfect these cells, as shown by high luciferase expression levels (108 to 109 relative light units per milligram of cell protein) that corresponded with 25–50% of green fluorescent protein-positive cells after 24 hours. However, unpredictable differences were observed among the vectors and cell types that a posteriori justified the screening procedure. We also showed that cells that were not transfected after the first experiment remained transfectable in a subsequent transfection experiment to a level similar to that of the initial population. This experiment does not support the emergence of a transfection-resistant cell population and opens the door to multiple therapeutic gene deliveries. Although efficacy and cell targeting still remain to be improved, PEI derivatives appear to be promising molecules for the development of nonviral gene therapy of ovarian carcinoma. [ABSTRACT FROM AUTHOR]

Published
2000
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58. Transient gene expression in mammalian cells grown in serum-free suspension culture.

Author

Schlaeger, Ernst-Jürgen and Christensen, Klaus

Abstract

In order to establish a simple and scaleable transfection system we have used the cationic polymer polyethylenimine (PEI) to study transient transfection in HEK293 and 293(EBNA) cells grown in serum-free suspension culture. The transfection complexes were made directly within the cell culture by consecutively adding plasmid and PEI (direct method). Alternatively, the DNA-PEI transfection complexes were prepared in fresh medium (1/10 culture volume) and then added to the cells (indirect method). The results of this study clearly show that the ratio of PEI nitrogen to DNA phosphate is very important for high expression levels. The precise ratio is dependent on the DNA concentration. For example, using 1 μg/ml DNA by the indirect method, the ratio of optimal PEI:DNA was about 10–13:1. However, the ratio increases to 33:1 for 0.1–0.2 μg/ml DNA. By testing several different molecular weights of the polycationic polymer we could show that the highest transfection efficiency was obtained with the PEI 25 kDa. Using PEI 25 kDa the indirect method is superior to the direct addition because significantly lower DNA concentrations are needed. The expression levels of the soluble human TNF receptor p55 are even higher at low DNA compared to 1 μg/ml plasmid. The EBV-based pREP vectors gave better transient gene expression when used in 293(EBNA) cells compared to HEK293 cells in suspension culture. No differences in expression levels in the two cell lines were observed when the pC1 (CMV)-TNFR was used. In conclusion, PEI is a low-toxic transfection agent which provides high levels of transient gene expression in 293(EBNA) cells grown in serum-free suspension culture. This system allows highly reproducible, cost-effective production of milligram amounts of recombinant proteins in 2–5 l spinner culture scale within 3–5 days. Fermentor scale experiments, however, are less efficient because the PEI-mediated transient tranfection is inhibited by conditioned medium. [ABSTRACT FROM AUTHOR]

Published
1999
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59. Macromolecular cytosolic delivery: Cell membranes as the primary obstacle.

Author

Larson, Gretchen and Lee, Kyung-Dall

Abstract

The “evolution” of a thing, a custom, an organ is thus by no means its progressus toward a goal, even less a logical progressus by the shortest route and with the least expenditure of force, but a succession of more of less profound, mutually independent processes of subduing, plus the resistances they encounter, the attempts at transformation for the purpose of defense and reaction, and the results of successful counteractions. The form is fluid, but the “meaning” is even more so (Friedrich W. Nietzsche). [ABSTRACT FROM AUTHOR]

Published
1998
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60. Author Index Volume 6 1999.

Subjects
AUTHORS, GENE therapy, PERIODICALS
Abstract

Lists authors of articles published in the volume 6, 1999 issue of the 'Gene Therapy' periodical. J. Abe; M. Abitbol; N. Accart; G.E. Blair.

Published
1999
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61. Hautgentherapie – Perspektiven des Gentransfers in Keratinozyten.

Author

Braun-Falco, Markus and Hallek, Michael

Abstract

Copyright of Der Hautarzt is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
1998
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62. Liposomes enhance delivery and expression of an RGD-oligolysine gene transfer vector in human tracheal cells.

Author

Colin, M, Harbottle, R P, Knight, A, Kornprobst, M, Cooper, R G, Miller, A D, Trugnan, G, Capeau, J, Coutelle, C, and Brahimi-Horn, M C

Subjects
GENETIC transformation, INTEGRINS, CYCLIC peptides, LIPOSOMES
Abstract

Nonviral gene delivery systems consist predominantly of lipoplexes or receptor-targeting and nontargeting polyplexes. We examined integrin-mediated gene delivery using an Arg-Gly-Asp/oligo-L-lysine ([K]16RGD) cyclic peptide and investigated its gene transfer efficiency when associated with a cationic liposome. We demonstrated that human cystic fibrosis and noncystic fibrosis tracheal epithelial cells in culture express integrins that recognise the RGD integrin-binding motif. We found a 10-fold (P < 0.01) increased expression of a luciferase encoding plasmid in these cells when complexing the plasmid to the [k]16RGD peptide as compared with plasmid alone. This increase was specific to the [K]16RGD peptide since neither a [K]16RGE nor a [K]16 peptide gave a comparable increase. Expression was further enhanced 30-fold (P < 0.01) with lipofectamine and the ratio of dna/peptide/lipofectamine was critical for specificity and expression. fluorescence and radioactive labelling of the complex showed that the [k]16RGD peptide increased the endocytic uptake of DNA into cells. The cell association of both DNA and peptide increased even further with lipofectamine. Confocal microscopy showed that the [K]16RGD peptide and the DNA internalised together within 30 min and localised to vesicles in the perinuclear region. These results show that an integrin-binding ligand can deliver genetic material to airway cells and that a cationic liposome can enhance the efficacy of this nonviral vector system. [ABSTRACT FROM AUTHOR]

Published
1998
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63. Gene delivery by negatively charged ternary complexes of DNA, cationic liposomes and transferrin or fusigenic peptides.

Author

Simões, S, Slepushkin, V, Gaspar, R, Pedroso de Lima, M C, and Düzgüneş, N

Subjects
GENE transfection, DNA, BETA-galactosidase
Abstract

Potential problems with the use of viral vectors for gene therapy necessitate the development of efficient nonviral vectors. The association of transferrin, or the pH-sensitive peptide GALA, with cationic liposomes composed of 1,2-dioleoyl-3-(trimethylammonium) propane and its equimolar mixture with dioleoylphosphatidylethanolamine, under conditions where the liposome/DNA complex is negatively charged, drastically increased luciferase expression from pCMVluc. The percentage of cells transfected, measured by β-galactosidase expression, was also increased by about 10-fold. The zeta potential of the ternary complexes was lower than that of the liposome/DNA complexes. Transfection activity of positively charged complexes was also enhanced by association with transferrin, GALA or the influenza hemagglutinin N terminal peptide HA-2, but to a smaller extent compared with the negatively charged complexes. The enhancement of gene delivery by transferrin or GALA was not affected significantly by the presence of serum and did not cause significant cytotoxicity. Our results indicate that negatively charged ternary complexes of cationic liposomes, DNA and transferrin, or fusigenic peptides, can facilitate efficient transfection of cultured cells, and that they may alleviate the drawbacks of the use of highly positively charged complexes for gene delivery in vivo. [ABSTRACT FROM AUTHOR]

Published
1998

64. Coupling of cell-binding ligands to polyethylenimine for targeted gene delivery.

Author

Kircheis, R, Kichler, A, Wallner, G, Kursa, M, Ogris, M, Felzmann, T, Buchberger, M, and Wagner, E

Subjects
POLYMERS, DNA, ENDOCYTOSIS
Abstract

Recently the high transfection potential of the cationic polymer polyethylenimine (PEI) was described (Boussif O et al. Proc Natl Acad Sci USA 1995; 92: 7297–7301). To combine the promising DNA delivering activity of PEI with the concept of receptor-mediated gene delivery, cell-binding ligands (transferrin or antiCD3 antibody) were incorporated by covalent linkage to PEI. DNA complexes of PEI or ligand-PEI conjugates were tested for transfection of cultured neuroblastoma Neuro 2A cells, melanoma B16 or H225 cells, erythroid leukemic K562 cells and T cell leukemia Jurkat E6.1 cells. Depending on the cell line, incorporation of the cell-binding ligand resulted in an up to 1000- fold increased transfection efficiency. This activity depends on ligand–receptor interaction and was observed also at low PEI cation:DNA anion ratios where ligand-free PEI lacks efficiency. Depending on the cell-binding ligand, specific targeting (CD3 antibody, Jurkat cells) can be achieved. Gene transfer can be augmented by the addition of an endosome-destabilizing influenza peptide, but is not dependent on the presence of additional endosomolytic agents. Application of transferrin-PEI for the production of murine interleukin-2 in B16 cells resulted in exceptionally high secretion rates of 19 μg IL-2 protein per 106 cells per 24 h. [ABSTRACT FROM AUTHOR]

Published
1997
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