Molecular Therapy: Nucleic Acids (Jun 2017)

Translation of Angiotensin-Converting Enzyme 2 upon Liver- and Lung-Targeted Delivery of Optimized Chemically Modified mRNA

  • Eva Schrom,
  • Maja Huber,
  • Manish Aneja,
  • Christian Dohmen,
  • Daniela Emrich,
  • Johannes Geiger,
  • Günther Hasenpusch,
  • Annika Herrmann-Janson,
  • Verena Kretzschmann,
  • Olga Mykhailyk,
  • Tamara Pasewald,
  • Prajakta Oak,
  • Anne Hilgendorff,
  • Dirk Wohlleber,
  • Heinz-Gerd Hoymann,
  • Dirk Schaudien,
  • Christian Plank,
  • Carsten Rudolph,
  • Rebekka Kubisch-Dohmen

DOI
https://doi.org/10.1016/j.omtn.2017.04.006
Journal volume & issue
Vol. 7, no. C
pp. 350 – 365

Abstract

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Changes in lifestyle and environmental conditions give rise to an increasing prevalence of liver and lung fibrosis, and both have a poor prognosis. Promising results have been reported for recombinant angiotensin-converting enzyme 2 (ACE2) protein administration in experimental liver and lung fibrosis. However, the full potential of ACE2 may be achieved by localized translation of a membrane-anchored form. For this purpose, we advanced the latest RNA technology for liver- and lung-targeted ACE2 translation. We demonstrated in vitro that transfection with ACE2 chemically modified messenger RNA (cmRNA) leads to robust translation of fully matured, membrane-anchored ACE2 protein. In a second step, we designed eight modified ACE2 cmRNA sequences and identified a lead sequence for in vivo application. Finally, formulation of this ACE2 cmRNA in tailor-made lipidoid nanoparticles and in lipid nanoparticles led to liver- and lung-targeted translation of significant amounts of ACE2 protein, respectively. In summary, we provide evidence that RNA transcript therapy (RTT) is a promising approach for ACE2-based treatment of liver and lung fibrosis to be tested in fibrotic disease models.

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