AI Article Synopsis

  • - Preclinical studies indicate that off-target effects from RNA interference contribute significantly to hepatotoxicity in GalNAc-siRNA conjugates.
  • - Researchers developed a new strategy called enhanced stabilization chemistry plus (ESC+) which effectively reduces off-target binding while preserving the intended on-target effects in RNA therapies.
  • - This approach was successfully applied to ALN-HBV, leading to a redesigned version (ALN-HBV02) with better specificity and safety, allowing it to resume clinical development.

Article Abstract

Preclinical mechanistic studies have pointed towards RNA interference-mediated off-target effects as a major driver of hepatotoxicity for GalNAc-siRNA conjugates. Here, we demonstrate that a single glycol nucleic acid or 2'-5'-RNA modification can substantially reduce small interfering RNA (siRNA) seed-mediated binding to off-target transcripts while maintaining on-target activity. In siRNAs with established hepatotoxicity driven by off-target effects, these novel designs with seed-pairing destabilization, termed enhanced stabilization chemistry plus (ESC+), demonstrated a substantially improved therapeutic window in rats. In contrast, siRNAs thermally destabilized to a similar extent by the incorporation of multiple DNA nucleotides in the seed region showed little to no improvement in rat safety suggesting that factors in addition to global thermodynamics play a role in off-target mitigation. We utilized the ESC+ strategy to improve the safety of ALN-HBV, which exhibited dose-dependent, transient and asymptomatic alanine aminotransferase elevations in healthy volunteers. The redesigned ALN-HBV02 (VIR-2218) showed improved specificity with comparable on-target activity and the program was reintroduced into clinical development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9262600PMC
http://dx.doi.org/10.1093/nar/gkac539DOI Listing

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