Abstract

ABSTRACT RNA interference (RNAi) is an ancient biological mechanism used to defend against external invasion. It theoretically can silence any disease-related genes in a sequence-specific manner, making small interfering RNA (siRNA) a promising therapeutic modality. After a two-decade journey from its discovery, two approvals of siRNA therapeutics, ONPATTRO ® (patisiran) and GIVLAARI™ (givosiran), have been achieved by Alnylam Pharmaceuticals. Reviewing the long-term pharmaceutical history of human beings, siRNA therapy currently has set up an extraordinary milestone, as it has already changed and will continue to change the treatment and management of human diseases. It can be administered quarterly, even twice-yearly, to achieve therapeutic effects, which is not the case for small molecules and antibodies. The drug development process was extremely hard, aiming to surmount complex obstacles, such as how to efficiently and safely deliver siRNAs to desired tissues and cells and how to enhance the performance of siRNAs with respect to their activity, stability, specificity and potential off-target effects. In this review, the evolution of siRNA chemical modifications and their biomedical performance are comprehensively reviewed. All clinically explored and commercialized siRNA delivery platforms, including the GalNAc ( N -acetylgalactosamine)–siRNA conjugate, and their fundamental design principles are thoroughly discussed. The latest progress in siRNA therapeutic development is also summarized. This review provides a comprehensive view and roadmap for general readers working in the field.

Keywords

Small interfering RNARNA interferenceComputational biologyMilestoneBiologyNanotechnologyMedicineBioinformaticsComputer scienceRNAGeneticsGene

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Year
2020
Type
review
Volume
5
Issue
1
Pages
101-101
Citations
1344
Access
Closed

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Bo Hu, Liping Zhong, Yuhua Weng et al. (2020). Therapeutic siRNA: state of the art. Signal Transduction and Targeted Therapy , 5 (1) , 101-101. https://doi.org/10.1038/s41392-020-0207-x

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DOI
10.1038/s41392-020-0207-x