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Dendritic amphiphilic siRNA: Selective albumin binding, in vivo efficacy, and low toxicityopen access

Authors
Fakih, Hassan H.Tang, QiSummers, AshleyShin, MinwookBuchwald, Julianna E.Gagnon, RosemaryHariharan, Vignesh N.Echeverria, DimasCooper, David A.Watts, Jonathan K.Khvorova, AnastasiaSleiman, Hanadi F.
Issue Date
Dec-2023
Publisher
Cell Press
Keywords
albumin; drug delivery; MT: Delivery Strategies; oligonucleotide therapeutics; protein binding; siRNAs
Citation
Molecular Therapy Nucleic Acids, v.34
Journal Title
Molecular Therapy Nucleic Acids
Volume
34
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/159589
DOI
10.1016/j.omtn.2023.102080
ISSN
2162-2531
Abstract
Although an increasing number of small interfering RNA (siRNA) therapies are reaching the market, the challenge of efficient extra-hepatic delivery continues to limit their full therapeutic potential. Drug delivery vehicles and hydrophobic conjugates are being used to overcome the delivery bottleneck. Previously, we reported a novel dendritic conjugate that can be appended efficiently to oligonucleotides, allowing them to bind albumin with nanomolar affinity. Here, we explore the ability of this novel albumin-binding conjugate to improve the delivery of siRNA in vivo. We demonstrate that the conjugate binds albumin exclusively in circulation and extravasates to various organs, enabling effective gene silencing. Notably, we show that the conjugate achieves a balance between hydrophobicity and safety, as it significantly reduces the side effects associated with siRNA interactions with blood components, which are commonly observed in some hydrophobically conjugated siRNAs. In addition, it reduces siRNA monocyte uptake, which may lead to cytokine/inflammatory responses. This work showcases the potential of using this dendritic conjugate as a selective albumin binding handle for the effective and safe delivery of nucleic acid therapeutics. We envision that these properties may pave the way for new opportunities to overcome delivery hurdles of oligonucleotides in future applications. © 2023
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