Oligonucleotide therapeutics (ONTs) are a growing class of nucleic acid–based therapies with the potential to treat a variety of diseases through several different mechanisms of action (MoA). The most prevalent MoA entails the inhibition of therapeutically relevant levels of protein expression via mRNA degradation, exemplified by numerous approved ONTs. ONTs have unique physicochemical properties, pharmacokinetic characteristics, and MoAs that are distinct from other drug classes. The result can be a disconnect between the administered dose, plasma drug concentrations, pharmacodynamics, and toxicity. Thus, ONT development poses unique scientific and regulatory challenges that are not fully addressed by current International Council for Harmonisation (ICH) guidelines. The complexity of ONT development has recently been recognized with the acceptance of the new ICH topic proposal “ICH S13—Nonclinical Safety Evaluation of Oligonucleotide-based Therapeutics.” In preparation for the ICH S13 Step 2 public consultation period, the International Consortium for Innovation and Quality in Pharmaceutical Development (IQ) DruSafe ONT Working Group convened to identify and discuss key considerations for ONT development, and to communicate areas where regulatory clarity and harmonization are most needed. Specifically, these include strategies to assess off-target toxicities, safety pharmacology, general toxicity studies, First-In-Human dose selection, genotoxicity studies, reproductive and developmental toxicity studies, carcinogenicity assessments, and the appropriate use of a surrogate molecule in development. The intended goals of this paper are to provide a means for communicating input towards the ICH process and to provide a resource for assisting with the public review of the draft ICH S13 Guidance.
RobertsTCLangerRWoodMJA. Advances in oligonucleotide drug delivery. Nat Rev Drug Discov. 2020;19(10):673-694. doi:10.1038/s41573-020-0075-7
2.
LaufferMCvan Roon-MomWAartsma-RusA. N = 1 collaborative. Possibilities and limitations of antisense oligonucleotide therapies for the treatment of monogenic disorders. Commun Med. 2024;4(1):6. doi:10.1038/s43856-023-00419-1
3.
AgrawalSZhangR. Pharmacokinetics of oligonucleotides. Ciba Found Symp. 1997;209:60-75. doi:10.1002/9780470515396.ch6; discussion 75-8.
4.
ShadidMBadawiMAbulrobA. Antisense oligonucleotides: absorption, distribution, metabolism, and excretion. Expert Opin Drug Metab Toxicol. 2021;17(11):1281-1292. doi:10.1080/17425255.2021
5.
YuBZhaoXLeeLJLeeRJ. Targeted delivery systems for oligonucleotide therapeutics. AAPS J. 2009;11(1):195-203. doi:10.1208/s12248-009-9096-1
6.
PaunovskaKLoughreyDDahlmanJE. Drug delivery systems for RNA therapeutics. Nat Rev Genet. 2022;23(5):265-280. doi:10.1038/s41576-021-00439-4
7.
HammondSMAartsma-RusAAlvesS, et al.Delivery of oligonucleotide-based therapeutics: challenges and opportunities. EMBO Mol Med. 2021;13(4):e13243. doi:10.15252/emmm.202013243
8.
SchubertDLevinAAKornbrustD, et al.The Oligonucleotide Safety Working Group (OSWG). Nucleic Acid Therapeut. 2012;22(4):211-212. doi:10.1089/nat.2012.0383
9.
International Council of Harmonisation. ICH M3(R2) Non-clinical safety studies for the conduct of human clinical trials for pharmaceuticals ‐ Scientific guideline. 2009.
10.
International Council of Harmonisation. ICH S6(R1) Preclinical safety evaluation of biotechnology-derived pharmaceuticals ‐ Scientific guideline. 2011.
11.
TessierYAchanzarWMihalcikL, et al.Outcomes of the European Federation of Pharmaceutical Industries and Associations Oligonucleotide Working Group Survey on Nonclinical Practices and Regulatory Expectations for Therapeutic Oligonucleotide Safety Assessment. Nucleic Acid Therapeut. 2021;31(1):7-20. doi:10.1089/nat.2020.0892
12.
EgliMManoharanM. Chemistry, structure and function of approved oligonucleotide therapeutics. Nucleic Acids Res. 2023;51(6):2529-2573. doi:10.1093/nar/gkad067
PMDA. Guideline for preclinical safety assessment of oligonucleotide therapeutics. 2020.
15.
Final Concept Paper S13 EWG: Non-clinical safety evaluation of oligonucleotide-based therapeutics In: ICH, editor. 2024.
16.
FDA. Nonclinical Safety Assessment of Oligonucleotide-Based Therapeutics. 2024.
17.
International Council of Harmonisation. ICH S9 Non-clinical evaluation for anticancer pharmaceuticals ‐ Scientific guideline. 2010.
18.
VinjamuriBPPanJPengP. A review on commercial oligonucleotide drug products. J Pharmacol Sci. 2024;113(7):1749-1768. doi:10.1016/j.xphs.2024.04.021
19.
FrazierKS. Antisense oligonucleotide therapies: the promise and the challenges from a toxicologic pathologist's perspective. Toixcol Pathol. 2015;43(1):78-89. https://pubmed.ncbi.nlm.nih.gov/25385330/
20.
AnderssonPBurelSAEstrellaH, et al.Assessing hybridization-dependent off-target risk for therapeutic oligonucleotides: updated industry recommendations. Nucleic Acid Therapeut. 2025;35(1):16-33. doi:10.1089/nat.2024.0072
21.
International Council of Harmonisation. Safety Pharmacology Studies for Human Pharmaceuticals S7A. 2001.
22.
International Council of Harmonisation. The non-clinical evaluation of the potential for delayed ventricular repolarization (QT interval prolongation) by human pharmaceuticals. 2005.
23.
BermanCLCannonKCuiY, et al.Recommendations for safety pharmacology evaluations of oligonucleotide-based therapeutics. Nucleic Acid Therapeut. 2014;24(4):291-301. doi:10.1089/nat.2013.0477
24.
QuYHendersonKAHarperTAJrVargasHM. Scientific review of the proarrhythmic risks of oligonucleotide therapeutics: are dedicated ICH S7B/E14 studies needed for low-risk modalities?Clin Pharmacol Ther. 2024;116(1):96-105. doi:10.1002/cpt.3204
25.
YuRZGunawanRGearyRSHughesSGHenrySPWangY. Lack of QT prolongation for 2'-O-methoxyethyl-modified antisense oligonucleotides based on retrospective exposure/response analysis of ten phase 1 dose-escalation placebo-controlled studies in healthy subjects. Nucleic Acid Therapeut. 2017;27(5):285-294. doi:10.1089/nat.2017.0676
26.
KallendDMasonJSmithPF, et al.An evaluation of a supratherapeutic dose of inclisiran on cardiac repolarization in healthy volunteers: a phase I, randomized study. Clin Transl Sci. 2022;15(11):2663-2672. doi:10.1111/cts.13391
27.
AyyarVSSongD. Mechanistic pharmacokinetics and pharmacodynamics of GalNAc-siRNA: translational model involving competitive receptor-mediated disposition and RISC-dependent gene silencing applied to givosiran. J Pharmacol Sci. 2024;113(1):176-190. doi:10.1016/j.xphs.2023.10.026
28.
BrownCRGuptaSQinJ, et al.Investigating the pharmacodynamic durability of GalNAc-siRNA conjugates. Nucleic Acids Res. 2020;48(21):11827-11844. doi:10.1093/nar/gkaa670
29.
GearyRSNorrisDYuRBennettCF. Pharmacokinetics, biodistribution and cell uptake of antisense oligonucleotides. Adv Drug Deliv Rev. 2015;87:46-51. doi:10.1016/j.addr.2015.01.008
30.
LehouxDKallendDWijngaardPLJBrownAPZerlerB. The N-Acetylgalactosamine-conjugated small interfering RNA inclisiran can be coadministered safely with atorvastatin in cynomolgus monkeys resulting in additive low-density lipoprotein cholesterol reductions. Pharmacol Res Perspect. 2023;11(2):e01080. doi:10.1002/prp2.1080
31.
JanasMMHarbisonCEPerryVK, et al.The nonclinical safety profile of GalNAc-conjugated RNAi therapeutics in subacute studies. Toxicol Pathol. 2018;46(7):735-745. doi:10.1177/0192623318792537
32.
HabtemariamBAKarstenVAttarwalaH, et al.Single-dose pharmacokinetics and pharmacodynamics of transthyretin targeting N-acetylgalactosamine-small interfering ribonucleic acid conjugate, vutrisiran, in healthy subjects. Clin Pharmacol Ther. 2021;109(2):372-382. doi:10.1002/cpt.1974
33.
RayKKRaalFJKallendDGORION Phase III investigators, et al.. ORION phase III investigators. Inclisiran and cardiovascular events: a patient-level analysis of phase III trials. Eur Heart J. 2023;44(2):129-138. doi:10.1093/eurheartj/ehac594
34.
DesaiASWebbDJTaubelJ, et al.Zilebesiran, an RNA interference therapeutic agent for hypertension. N Engl J Med. 2023;389(3):228-238. doi:10.1056/NEJMoa2208391
35.
GosselinNHSchuckVJABarriereO, et al.Translational population-pharmacodynamic modeling of a novel long-acting siRNA therapy, inclisiran, for the treatment of hypercholesterolemia. Clin Pharmacol Ther. 2023;113(2):328-338. doi:10.1002/cpt.2774
36.
ParryJDHarperTAJrAnderssonP, et al.Opportunities for more tailored approaches to genotoxicity testing and carcinogenicity strategy for oligonucleotide therapeutics: outcome of an industry survey. Nucleic Acid Therapeut. 2025;35(1):34-48. doi:10.1089/nat.2024.0075
37.
HenrySPMonteithDKMatsonJE, et al.Assessment of the genotoxic potential of ISIS 2302: a phosphorothioate oligodeoxynucleotide. Mutagenesis. 2002;17(3):201-209. doi:10.1093/mutage/17.3.201
38.
BermanCLBarrosSAGallowaySM, et al.OSWG recommendations for genotoxicity testing of novel oligonucleotide-based therapeutics. Nucleic Acid Therapeut. 2016;26(2):73-85. doi:10.1089/nat.2015.0534
39.
JanasMMJiangYDuncanRG, et al.Exposure to siRNA-GalNAc conjugates in systems of the standard test battery for genotoxicity. Nucleic Acid Therapeut. 2016;26(6):363-371. doi:10.1089/nat.2016.0622
40.
GuérardMAndreasZErichK, et al.Locked nucleic acid (LNA): based single-stranded oligonucleotides are not genotoxic. Environ Mol Mutagen. 2017;58(3):112-121. doi:10.1002/em.22076
41.
International Council of Harmonisation. Guidance for genotoxicity testing and data interpretation for pharmaceuticals intended for human use S2(R1). 2012.
42.
HannasBRBenderSMBlasiE, et al.Developmental and reproductive toxicity testing strategies for oligonucleotides: a workshop proceedings. Nucleic Acid Therapeut. 2025;35(3):93-113. doi:10.1089/nat.2025.0013
43.
CavagnaroJBermanCKornbrustDWhiteTCampionSHenryS. Considerations for assessment of reproductive and developmental toxicity of oligonucleotide-based therapeutics. Nucleic Acid Therapeut. 2014;24(5):313-325. doi:10.1089/nat.2014.0490
44.
International Council of Harmonisation. Detection of reproductive and developmental toxicity for human pharmaceuticals S5(R3). 2020.
45.
International Council of Harmonisation. Testing for carcinogenicity of pharmaceuticals S1B(R1). 2022.
46.
VahleJLDybowskiJGrazianoM, et al.ICH S1 prospective evaluation study and weight of evidence assessments: commentary from industry representatives. Front Toxicol. 2024;6:1377990. doi:10.3389/ftox.2024.1377990
47.
AupyPEchevarríaLRelizaniK, et al.Identifying and avoiding tcDNA-ASO sequence-specific toxicity for the development of DMD exon 51 skipping therapy. Mol Ther Nucleic Acids. 2020;19:371-383. doi:10.1016/j.omtn.2019.11.020
48.
FarmanCAKornbrustDJ. Oligodeoxynucleotide studies in primates: antisense and immune stimulatory indications. Toxicol Pathol. 2003;31(Suppl):119-122. doi:10.1080/01926230390174995
49.
ShenLFrazer-AbelAReynoldsPR, et al.Mechanistic understanding for the greater sensitivity of monkeys to antisense oligonucleotide-mediated complement activation compared with humans. J Pharmacol Exp Therapeut. 2014;351(3):709-717. doi:10.1124/jpet.114.219378
50.
ShenLWongAOnedaS, et al.Complement C3d/C4d deposition on platelets correlates with 2'-O-methoxyethyl antisense oligonucleotide-induced thrombocytopenia in monkeys. Nucleic Acid Therapeut. 2023;33(3):209-225. doi:10.1089/nat.2022.0042
51.
FlierlUNeroTLLimB, et al.Phosphorothioate backbone modifications of nucleotide-based drugs are potent platelet activators. J Exp Med. 2015;212(2):129-137. doi:10.1084/jem.20140391
