Small interfering RNA: Discovery, pharmacology and clinical development-An introductory review

Priyanga Ranasinghe; Melisande L Addison; James W Dear; David J Webb

doi:10.1111/bph.15972

Small interfering RNA: Discovery, pharmacology and clinical development-An introductory review

Br J Pharmacol. 2023 Nov;180(21):2697-2720. doi: 10.1111/bph.15972. Epub 2022 Nov 13.

Authors

Priyanga Ranasinghe^{1

2}, Melisande L Addison², James W Dear², David J Webb²

Affiliations

¹ Department of Pharmacology, Faculty of Medicine, University of Colombo, Colombo, Sri Lanka.
² University/British Heart Foundation Centre for Cardiovascular Science, The University of Edinburgh, Edinburgh, UK.

PMID: 36250252
DOI: 10.1111/bph.15972

Abstract

Post-transcriptional gene silencing targets and degrades mRNA transcripts, silencing the expression of specific genes. RNA interference technology, using synthetic structurally well-defined short double-stranded RNA (small interfering RNA [siRNA]), has advanced rapidly in recent years. This introductory review describes the utility of siRNA, by exploring the underpinning biology, pharmacology, recent advances and clinical developments, alongside potential limitations and ongoing challenges. Mediated by the RNA-induced silencing complex, siRNAs bind to specific complementary mRNAs, which are subsequently degraded. siRNA therapy offers advantages over other therapeutic approaches, including ability of specifically designed siRNAs to potentially target any mRNA and improved patient adherence through infrequent administration associated with a very long duration of action. Key pharmacokinetic and pharmacodynamic challenges include targeted administration, poor tissue penetration, nuclease inactivation, rapid renal elimination, immune activation and off-target effects. These have been overcome by chemical modification of siRNA and/or by utilising a range of delivery systems, increasing bioavailability and stability to allow successful clinical translation. Patisiran (hereditary transthyretin-mediated amyloidosis) was the first licensed siRNA, followed by givosiran (acute hepatic porphyria), lumasiran (primary hyperoxaluria type 1) and inclisiran (familial hypercholesterolaemia), which all use N-acetylgalactosamine (GalNAc) linkage for effective liver-directed delivery. Others are currently under development for indications varying from rare genetic diseases to common chronic non-communicable diseases (hypertension, cancer). Technological advances are paving the way for broader clinical use. Ongoing challenges remain in targeting organs beyond the liver and reaching special sites (e.g., brain). By overcoming these barriers, siRNA therapy has the potential to substantially widen its therapeutic impact.

Keywords: RNA interference; medication adherence; post-transcriptional gene silencing; siRNA; therapeutics.

Publication types

Review

MeSH terms

Humans
Porphyrias, Hepatic* / drug therapy
Porphyrias, Hepatic* / genetics
RNA Interference
RNA, Double-Stranded*
RNA, Messenger
RNA, Small Interfering / genetics

Substances

RNA, Double-Stranded
RNA, Small Interfering
RNA, Messenger