Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery

Irene Martin; Christian Dohmen; Carlos Mas-Moruno; Christina Troiber; Petra Kos; David Schaffert; Ulrich Lächelt; Meritxell Teixidó; Michael Günther; Horst Kessler; Ernest Giralt; Ernst Wagner

doi:10.1039/c2ob06907e

Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery

Irene Martin, Christian Dohmen, Carlos Mas-Moruno, Christina Troiber, Petra Kos, David Schaffert, Ulrich Lächelt, Meritxell Teixidó, Michael Günther, Horst Kessler, Ernest Giralt, Ernst Wagner

TUM Emeriti of Excellence

Research output: Contribution to journal › Article › peer-review

64 Scopus citations

Abstract

In the forthcoming era of cancer gene therapy, efforts will be devoted to the development of new efficient and non-toxic gene delivery vectors. In this regard, the use of Fmoc/Boc-protected oligo(ethane amino)acids as building blocks for solid-phase-supported assembly represents a novel promising approach towards fully controlled syntheses of effective gene vectors. Here we report on the synthesis of defined polymers containing the following: (i) a plasmid DNA (pDNA) binding domain of eight succinoyl-tetraethylenpentamine (Stp) units and two terminal cysteine residues; (ii) a central polyethylene glycol (PEG) chain (with twenty-four oxyethylene units) for shielding; and (iii) specific peptides for targeting towards cancer cells. Peptides B6 and c(RGDfK), which bind transferrin receptor and α _vβ ₃ integrin, respectively, were chosen because of the high expression of these receptors in many tumoral cells. This study shows the feasibility of designing these kinds of fully controlled vectors and their success for targeted pDNA-based gene transfer.

Original language	English
Pages (from-to)	3258-3268
Number of pages	11
Journal	Organic and Biomolecular Chemistry
Volume	10
Issue number	16
DOIs	https://doi.org/10.1039/c2ob06907e
State	Published - 28 Apr 2012

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Martin, I., Dohmen, C., Mas-Moruno, C., Troiber, C., Kos, P., Schaffert, D., Lächelt, U., Teixidó, M., Günther, M., Kessler, H., Giralt, E., & Wagner, E. (2012). Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery. Organic and Biomolecular Chemistry, 10(16), 3258-3268. https://doi.org/10.1039/c2ob06907e

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title = "Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery",

abstract = "In the forthcoming era of cancer gene therapy, efforts will be devoted to the development of new efficient and non-toxic gene delivery vectors. In this regard, the use of Fmoc/Boc-protected oligo(ethane amino)acids as building blocks for solid-phase-supported assembly represents a novel promising approach towards fully controlled syntheses of effective gene vectors. Here we report on the synthesis of defined polymers containing the following: (i) a plasmid DNA (pDNA) binding domain of eight succinoyl-tetraethylenpentamine (Stp) units and two terminal cysteine residues; (ii) a central polyethylene glycol (PEG) chain (with twenty-four oxyethylene units) for shielding; and (iii) specific peptides for targeting towards cancer cells. Peptides B6 and c(RGDfK), which bind transferrin receptor and α vβ 3 integrin, respectively, were chosen because of the high expression of these receptors in many tumoral cells. This study shows the feasibility of designing these kinds of fully controlled vectors and their success for targeted pDNA-based gene transfer.",

author = "Irene Martin and Christian Dohmen and Carlos Mas-Moruno and Christina Troiber and Petra Kos and David Schaffert and Ulrich L{\"a}chelt and Meritxell Teixid{\'o} and Michael G{\"u}nther and Horst Kessler and Ernest Giralt and Ernst Wagner",

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Martin, I, Dohmen, C, Mas-Moruno, C, Troiber, C, Kos, P, Schaffert, D, Lächelt, U, Teixidó, M, Günther, M, Kessler, H, Giralt, E & Wagner, E 2012, 'Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery', Organic and Biomolecular Chemistry, vol. 10, no. 16, pp. 3258-3268. https://doi.org/10.1039/c2ob06907e

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AU - Martin, Irene

AU - Dohmen, Christian

AU - Mas-Moruno, Carlos

AU - Troiber, Christina

AU - Kos, Petra

AU - Schaffert, David

AU - Lächelt, Ulrich

AU - Teixidó, Meritxell

AU - Günther, Michael

AU - Kessler, Horst

AU - Giralt, Ernest

AU - Wagner, Ernst

PY - 2012/4/28

Y1 - 2012/4/28

N2 - In the forthcoming era of cancer gene therapy, efforts will be devoted to the development of new efficient and non-toxic gene delivery vectors. In this regard, the use of Fmoc/Boc-protected oligo(ethane amino)acids as building blocks for solid-phase-supported assembly represents a novel promising approach towards fully controlled syntheses of effective gene vectors. Here we report on the synthesis of defined polymers containing the following: (i) a plasmid DNA (pDNA) binding domain of eight succinoyl-tetraethylenpentamine (Stp) units and two terminal cysteine residues; (ii) a central polyethylene glycol (PEG) chain (with twenty-four oxyethylene units) for shielding; and (iii) specific peptides for targeting towards cancer cells. Peptides B6 and c(RGDfK), which bind transferrin receptor and α vβ 3 integrin, respectively, were chosen because of the high expression of these receptors in many tumoral cells. This study shows the feasibility of designing these kinds of fully controlled vectors and their success for targeted pDNA-based gene transfer.

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Solid-phase-assisted synthesis of targeting peptide-PEG-oligo(ethane amino)amides for receptor-mediated gene delivery

Abstract

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