Guanabenz (Wytensin™) selectively enhances uptake and efficacy of hydrophobically modified siRNAs

Osborn, Maire F.; Alterman, Julia F.; Nikan, Mehran; Cao, Hong; Didiot, Marie Cécile; Hassler, Matthew R.; Coles, Andrew H.; Khvorova, Anastasia

doi:10.1093/nar/gkv942

Cited by 40 publications

(28 citation statements)

References 30 publications

(36 reference statements)

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“…However, further analysis of structure activity relationships may lead to the development of new compounds with greater efficacy and reduced toxicity. It is interesting to note that other groups have begun to describe oligonucleotide enhancing small molecules (28, 29) . The structures of those molecules are very different from ones described here or previously by us (20) , suggesting that there may be a variety of mechanisms by which small molecules can augment effects of oligonucleotides.…”

Section: Resultsmentioning

confidence: 99%

A Novel Family of Small Molecules that Enhance the Intracellular Delivery and Pharmacological Effectiveness of Antisense and Splice Switching Oligonucleotides

Wang¹,

Ariyarathna

Xin

et al. 2017

ACS Chem. Biol.

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The pharmacological effectiveness of oligonucleotides has been hampered by their tendency to remain entrapped in endosomes thus limiting their access to cytosolic or nuclear targets. We have previously reported a group of small molecules that enhance the effects of oligonucleotides by causing their release from endosomes. Here we describe a second novel family of oligonucleotide enhancing compounds (OECs) that is chemically distinct from the compounds reported previously. We demonstrate that these molecules substantially augment the actions of splice switching oligonucleotides (SSOs) and antisense oligonucleotides (ASOs) in cell culture. We also find enhancement of SSO effects in a murine model. These new compounds act by increasing endosome permeability and causing partial release of entrapped oligonucleotides. While they also affect the permeability of lysosomes, they are clearly different from typical lysosomotropic agents. Current members of this compound family display a relatively narrow window between effective dose and toxic dose. Thus further improvements are necessary before these agents can become suitable for therapeutic use.

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Section: Resultsmentioning

confidence: 99%

A Novel Family of Small Molecules that Enhance the Intracellular Delivery and Pharmacological Effectiveness of Antisense and Splice Switching Oligonucleotides

Wang¹,

Ariyarathna

Xin

et al. 2017

ACS Chem. Biol.

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“…Other studies have investigated the use of small molecules for enhancing knockdown mediated by chol-siRNA and LNP-siRNA [19][20][21][22] . In these studies, the identified small molecules acted through either facilitating uptake or by effects on intracellular processes-potentially including endosomal escape.…”

Section: Discussionmentioning

confidence: 99%

“…While release-enhancing strategies using endosmolytic polymers or peptides have been promising 17,18 , such approaches are challenging from a formulation, toxicity, and bioavailability perspective. Efforts have also been made to identify small-molecule drugs capable of enhancing oligonucleotide delivery [19][20][21][22] . However, direct visualization or analysis of enhanced endosomal escape of non-formulated oligonucleotides has not been possible.…”

mentioning

confidence: 99%

Imaging small molecule-induced endosomal escape of siRNA

et al. 2020

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Small interfering RNAs (siRNAs) are a new class of promising therapeutic molecules that can be used for sequence-specific downregulation of disease-causing genes. However, endosomal entrapment of siRNA is a key hurdle for most delivery strategies, limiting the therapeutic effect. Here, we use live-cell microscopy and cytosolic galectin-9 as a sensor of membrane damage, to probe fundamental properties of endosomal escape of cholesterol-conjugated siRNA induced by endosome-disrupting compounds. We demonstrate efficient release of ligand-conjugated siRNA from vesicles damaged by small molecules, enhancing target knockdown up to ∼47-fold in tumor cells. Still, mismatch between siRNA-containing and drug-targeted endolysosomal compartments limits siRNA activity improvement. We also show widespread endosomal damage in macroscopic tumor spheroids after small molecule treatment, substantially improving siRNA delivery and knockdown throughout the spheroid. We believe the strategy to characterize endosomal escape presented here will be widely applicable, facilitating efforts to improve delivery of siRNA and other nucleic acid-based therapeutics.

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“…16,33 In fact, the small-molecule GSK-3 inhibitor CHIR99021 also increased SSO activity in HeLa-EGFP-654 cells ( Figure 7A). Via the use of small molecules identified in similar high-throughput screens, 17,58,59 it has previously been observed that the silencing ability of ASOs and hydrophobically modified siRNAs can be augmented through effective release from the late endosome. However, at the present time it remains an open question as to precisely how 6BIO augments ASO activity.…”

Section: Discussionmentioning

confidence: 99%

6BIO Enhances Oligonucleotide Activity in Cells: A Potential Combinatorial Anti-androgen Receptor Therapy in Prostate Cancer Cells

et al. 2017

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Guanabenz (Wytensin™) selectively enhances uptake and efficacy of hydrophobically modified siRNAs

Cited by 40 publications

References 30 publications

A Novel Family of Small Molecules that Enhance the Intracellular Delivery and Pharmacological Effectiveness of Antisense and Splice Switching Oligonucleotides

A Novel Family of Small Molecules that Enhance the Intracellular Delivery and Pharmacological Effectiveness of Antisense and Splice Switching Oligonucleotides

Imaging small molecule-induced endosomal escape of siRNA

6BIO Enhances Oligonucleotide Activity in Cells: A Potential Combinatorial Anti-androgen Receptor Therapy in Prostate Cancer Cells

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