Chemical Modifications to Improve the Cellular Uptake of Oligonucleotides

Debart, Françoise; Abes, Saïd; Deglane, Gaëlle; Moulton, Hong M.; Clair, Philippe; Gait, Michael J.; Vasseur, Jean‐Jacques; Lebleu, Bernard

doi:10.2174/156802607780487704

Cited by 48 publications

(26 citation statements)

References 115 publications

(124 reference statements)

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“…S1-S7). This is consistent with reports that show that endosomal release of CPP-cargo conjugates is sometimes very inefficient, one factor that currently limits their utility for macromolecular cargo delivery (19,25,29,30). Another factor that can limit the utility of cationic CPPs is that they do not enter cells that are not capable of endocytosis.…”

Section: Discussionsupporting

confidence: 90%

“…Once endocytosed, there is the complicating question of cargo release from endosomes that has sometimes been attributed to spontaneous membrane translocation (16). As we show below, endosomal release can be very inefficient (19,25,29,30) and can effectively prevent the delivery of some endocytosed cargos to the cytosol. Given this roadblock to delivery, various approaches based on physical or osmotic lysis of endosomes have been tested to increase the efficiency of endosomal release postuptake (22,29,(31)(32)(33)(34).…”

mentioning

confidence: 82%

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Direct Cytosolic Delivery of Polar Cargo to Cells by Spontaneous Membrane-translocating Peptides

He¹,

Kauffman²,

Fuselier³

et al. 2013

Journal of Biological Chemistry

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Background: Spontaneous membrane-translocating peptides were discovered by screening in synthetic lipid vesicles. Results: The translocating peptides carry membrane-impermeant cargos directly across cell membranes and drive systemic biodistribution in small animals. Conclusion: These peptides constitute a new class of delivery vehicle for membrane-impermeant cargos. Significance: Spontaneous membrane-translocating peptides could expand the universe of useful drugs.

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Section: Discussionsupporting

confidence: 90%

mentioning

confidence: 82%

Direct Cytosolic Delivery of Polar Cargo to Cells by Spontaneous Membrane-translocating Peptides

He¹,

Kauffman²,

Fuselier³

et al. 2013

Journal of Biological Chemistry

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“…Chemical modifications have been found to reduce the immune stimulatory capability of RNA duplexes (Morrissey et al 2005;Behlke 2008;Judge and MacLachlan 2008;Watts et al 2008;Robbins et al 2009). Chemical modifications have also been developed to improve pharmacological properties of siRNAs, including stability against nucleases found in biological fluids and improved cellular uptake (Bumcrot et al 2006;Debart et al 2007).…”

Section: Introductionmentioning

confidence: 99%

Effects of chemical modification on the potency, serum stability, and immunostimulatory properties of short shRNAs

Ge¹,

Dallas²,

Ilves³

et al. 2009

RNA

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Small hairpin RNAs (shRNAs) with 19-base-pair, or shorter, stems (short shRNAs [sshRNAs]) have been found to constitute a class whose mechanism of action appears to be distinct from that of small interfering RNAs (siRNAs) or longer shRNAs. These sshRNAs can be as active as canonical siRNAs or longer shRNAs. Their activity is affected by whether the antisense strand is positioned 59 or 39 to the loop (L or R sshRNAs, respectively). Dicer seems not to be involved in the processing of sshRNAs, although the mechanism of target gene suppression by these hairpins is through Ago2-mediated mRNA cleavage. In this study, the effects of chemical modifications on the potency, serum stability, and innate immune response of sshRNAs were investigated. Deoxynucleotide substitution and 29-O-methyl (29-OMe) modification in the sense strand and loop did not affect silencing activity, but, unlike with siRNAs, when placed in the antisense strand these modifications were detrimental. Conjugation with bulky groups at the 59-end of L sshRNAs or 39-end of R sshRNAs had a negative impact on the potency. Unmodified sshRNAs in dimer form or with blunt ends were immunostimulatory. Some modifications such as 39-end conjugation and phosphorothioate linkages on the backbone of the sshRNAs could also induce inflammatory cytokine production. However, 29-OMe substitution of sshRNAs abrogated the innate immune response and improved the serum stability of the hairpins.

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“…The combination of nucleotides with aminoalkyl chains greatly enhances the variety of possible structures as well as their potential application [24]. Thus, oligonucleotides possessing cationic functionalities in addition to the anionic phosphate backbone have been shown to exhibit promising properties [25][26][27][28]. Polyamines, putrescine, spermine and spermidine, are involved in the regulation of gene function [29,30].…”

Section: Introductionmentioning

confidence: 99%

Non-Nucleosidic Analogues of Polyaminonucleosides and Their Influence on Thermodynamic Properties of Derived Oligonucleotides

Brzezinska

Markiewicz

2015

Molecules

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Abstract:The rationale for the synthesis of cationic modified nucleosides is higher expected nuclease resistance and potentially better cellular uptake due to an overall reduced negative charge based on internal charge compensation. Due to the ideal distance between cationic groups, polyamines are perfect counterions for oligodeoxyribonucleotides. We have synthesized non-nucleosidic analogues built from units that carry different diol structures instead of sugar residues and functionalized with polyamines. The non-nucleosidic analogues were attached as internal or 5′-terminal modifications in oligodeoxyribonucleotide strands. The thermodynamic studies of these polyaminooligonucleotide analogues revealed stabilizing or destabilizing effects that depend on the linker or polyamine used.

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Chemical Modifications to Improve the Cellular Uptake of Oligonucleotides

Cited by 48 publications

References 115 publications

Direct Cytosolic Delivery of Polar Cargo to Cells by Spontaneous Membrane-translocating Peptides

Direct Cytosolic Delivery of Polar Cargo to Cells by Spontaneous Membrane-translocating Peptides

Effects of chemical modification on the potency, serum stability, and immunostimulatory properties of short shRNAs

Non-Nucleosidic Analogues of Polyaminonucleosides and Their Influence on Thermodynamic Properties of Derived Oligonucleotides

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