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Chemically modified RNA induces osteogenesis of stem cells and human tissue explants as well as accelerates bone healing in rats

  • Elizabeth R. Balmayor
  • , Johannes P. Geiger
  • , Manish K. Aneja
  • , Taras Berezhanskyy
  • , Maximilian Utzinger
  • , Olga Mykhaylyk
  • , Carsten Rudolph
  • , Christian Plank
  • Technical University of Munich
  • ethris GmbH

Research output: Contribution to journalArticlepeer-review

104 Scopus citations

Abstract

Limitations associated to the use of growth factors represent a major hurdle to musculoskeletal regeneration. On the one hand, they are needed to induce neo-tissue formation for the substitution of a necrotic or missing tissue. On the other hand, these factors are used in supraphysiological concentrations, are short lived and expensive and result in many side effects. Here we develop a gene transfer strategy based on the use of chemically modified mRNA (cmRNA) coding for human bone morphogenetic protein 2 (hBMP-2) that is non-immunogenic and highly stable when compared to unmodified mRNA. Transfected stem cells secrete hBMP-2, show elevated alkaline phosphatase levels and upregulated expression of RunX2, ALP, Osterix, Osteocalcin, Osteopontin and Collagen Type I genes. Mineralization was induced as seen by positive Alizarin red staining. hBMP-2 cmRNA transfected human fat tissue also yielded an osteogenic response in vitro as indicated by expression of hBMP-2, RunX2, ALP and Collagen Type I. Delivering hBMP-2 cmRNA to a femur defect in a rat model results in new bone tissue formation as early as 2 weeks after application of very low doses. Overall, our studies demonstrate the feasibility and therapeutic potential of a new cmRNA-based gene therapy strategy that is safe and efficient. When applied clinically, this approach could overcome BMP-2 growth factor associated limitations in bone regeneration.

Original languageEnglish
Pages (from-to)131-146
Number of pages16
JournalBiomaterials
Volume87
DOIs
StatePublished - 1 May 2016

Keywords

  • Bone healing
  • Bone morphogenetic protein
  • Chemically modified mRNA
  • Genetically modified fat graft
  • In vitro osteogenesis
  • MRNA delivery

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