Hydroxyproline-based DNA mimics provide an efficient gene silencing in vitro and in vivo

Ефимов, В. А.; Birikh, Klara R.; Staroverov, Dmitry B; Lukyanov, S. A.; Tereshina, Maria B.; Zaraisky, Andrey G.; Chakhmakhcheva, O. G.

doi:10.1093/nar/gkl249

Cited by 16 publications

(10 citation statements)

References 38 publications

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“…In the present study, we have elaborated a strategy combining a non-covalent peptide-based delivery system and a charged PNA-like DNA mimic that is likely to have potent implications i n therapeutics. HypNA- p PNA DNA mimics have already been used successfully both in vitro and in vivo (19,20,31,32) and offer several advantages due to their tight interaction with target DNA as well as their high solubility (21,32). Cell-penetrating peptides are most promising tools for delivery of therapeutic molecules (8,9) and the recent reconsideration of their cellular uptake mechanism has provided new perspectives for their in vivo application (25,26).…”

Section: Discussionmentioning

confidence: 99%

A non-covalent peptide-based carrier for in vivo delivery of DNA mimics

Morris

Gros

Aldrian

et al. 2007

Nucleic Acids Research

113

103

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The dramatic acceleration in identification of new nucleic-acid-based therapeutic molecules has provided new perspectives in pharmaceutical research. However, their development is limited by their poor cellular uptake and inefficient trafficking. Here we describe a short amphipathic peptide, Pep-3, that combines a tryptophan/phenylalanine domain with a lysine/arginine-rich hydrophilic motif. Pep-3 forms stable nano-size complexes with peptide-nucleic acid analogues and promotes their efficient delivery into a wide variety of cell lines, including primary and suspension lines, without any associated cytotoxicity. We demonstrate that Pep-3-mediated delivery of antisense-cyclin B1-charged-PNA blocks tumour growth in vivo upon intratumoral and intravenous injection. Moreover, we show that PEGylation of Pep-3 significantly improves complex stability in vivo and consequently the efficiency of antisense cyclin B1 administered intravenously. Given the biological characteristics of these vectors, we believe that peptide-based delivery technologies hold a true promise for therapeutic applications of DNA mimics.

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Section: Discussionmentioning

confidence: 99%

A non-covalent peptide-based carrier for in vivo delivery of DNA mimics

Morris

Gros

Aldrian

et al. 2007

Nucleic Acids Research

113

103

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“…(7) [107]. These compounds have been proved to be able to perform efficient gene silencing in vitro and in vivo [108]. It is interesting that the 3'-equivalent and 5' equivalent of these compounds match with the model proposed in Fig.…”

Section: Dna Binding By Cyclic Pnasmentioning

confidence: 89%

“…In fact the best performing trans-L-isomers were chosen for the biological tests. Cell-free experiments showed the ability of these compounds to inhibit translation with antisense mechanism (as tested by inhibiting luciferase activity in cellular extracts) [108]. These compounds were found to be able to penetrate into HS-68 and HeLa cells with cytoplasmatic distribution [37,108].…”

Section: Effect Of Cyclic Pnas In Cellular and Animal Systemsmentioning

confidence: 99%

“…Cell-free experiments showed the ability of these compounds to inhibit translation with antisense mechanism (as tested by inhibiting luciferase activity in cellular extracts) [108]. These compounds were found to be able to penetrate into HS-68 and HeLa cells with cytoplasmatic distribution [37,108]. Furthermore, they were shown to be effectively delivered into eukaryotic cells using lipofectamine (LFA) transfection, with maximum uptake after 20-24 h [108].…”

Section: Effect Of Cyclic Pnas In Cellular and Animal Systemsmentioning

confidence: 99%

“…These compounds were found to be able to penetrate into HS-68 and HeLa cells with cytoplasmatic distribution [37,108]. Furthermore, they were shown to be effectively delivered into eukaryotic cells using lipofectamine (LFA) transfection, with maximum uptake after 20-24 h [108]. This approach is possible with these compounds since they are negatively charged and can interact with the cationic carrier.…”

Section: Effect Of Cyclic Pnas In Cellular and Animal Systemsmentioning

confidence: 99%

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Peptide Nucleic Acids with a Structurally Biased Backbone: Effects of Conformational Constraints and Stereochemistry

Corradini¹,

Sforza²,

Tedeschi³

et al. 2007

CTMC

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Peptide nucleic acids (PNAs) are polyamidic oligonucleotide analogs which have been described for the first time fifteen years ago and were immediately found to be excellent tools in binding DNA and RNA for diagnostics and gene regulation. Their use as therapeutic agents have been proposed since early studies and recent advancements in cellular delivery systems, and in the so called anti-gene strategy, makes them good candidates for drug development. The search for new chemical modification of PNAs is a very active field of research and new structures are continuously proposed. This review focuses on the recent advancements obtained by the modification of the PNA backbone, and their possible use in medicinal chemistry. In particular two classes of structurally biased PNAs are described in details: i) PNAs with acyclic structures and their helical preference, which is regulated by stereochemistry and ii) cyclic PNAs with preorganized structures, whose performances depend both on stereochemistry and on conformational constraints. The properties of these compounds are discussed in terms of affinity for nucleic acids, and several recent examples of their use in cellular or animal systems are presented.

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Cellular Bioavailability of Peptide Nucleic Acids (PNAs) Conjugated to Cell Penetrating Peptides

Shiraishi

Nielsen

2009

Delivery Technologies for Biopharmaceuticals

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Hydroxyproline-based DNA mimics provide an efficient gene silencing in vitro and in vivo

Cited by 16 publications

References 38 publications

A non-covalent peptide-based carrier for in vivo delivery of DNA mimics

A non-covalent peptide-based carrier for in vivo delivery of DNA mimics

Peptide Nucleic Acids with a Structurally Biased Backbone: Effects of Conformational Constraints and Stereochemistry

Cellular Bioavailability of Peptide Nucleic Acids (PNAs) Conjugated to Cell Penetrating Peptides

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