Molecular Therapy: Nucleic Acids (Jun 2019)

Modeling the Kinetics of Lipid-Nanoparticle- Mediated Delivery of Multiple siRNAs to Evaluate the Effect on Competition for Ago2

  • Radu Mihaila,
  • Dipali Ruhela,
  • Beverly Galinski,
  • Ananda Card,
  • Mark Cancilla,
  • Timothy Shadel,
  • Jing Kang,
  • Samnang Tep,
  • Jie Wei,
  • R. Matthew Haas,
  • Jeremy Caldwell,
  • W. Michael Flanagan,
  • Nelly Kuklin,
  • Elena Cherkaev,
  • Brandon Ason

Journal volume & issue
Vol. 16
pp. 367 – 377

Abstract

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Drug combinations can improve the control of diseases involving redundant and highly regulated pathways. Validating a multi-target therapy early in drug development remains difficult. Small interfering RNAs (siRNAs) are routinely used to selectively silence a target of interest. Owing to the ease of design and synthesis, siRNAs hold promise for combination therapies. Combining siRNAs against multiple targets remains an attractive approach to interrogating highly regulated pathways. Currently, questions remain regarding how broadly such an approach can be applied, since siRNAs have been shown to compete with one another for binding to Argonaute2 (Ago2), the protein responsible for initiating siRNA-mediated mRNA degradation. Mathematical modeling, coupled with in vitro and in vivo experiments, led us to conclude that endosomal escape kinetics had the highest impact on Ago2 depletion by competing lipid-nanoparticle (LNP)-formulated siRNAs. This, in turn, affected the level of competition observed between them. A future application of this model would be to optimize delivery of desired siRNA combinations in vitro to attenuate competition and maximize the combined therapeutic effect. Keywords: RNA interference, siRNA, lipid nanoparticles, combination therapy, competition, mathematical modeling