Efficient healing of large osseous segmental defects using optimized chemically modified messenger RNA encoding BMP-2

Author:

De La Vega Rodolfo E.12ORCID,van Griensven Martijn12ORCID,Zhang Wen3,Coenen Michael J.1,Nagelli Christopher V.1ORCID,Panos Joseph A.1,Peniche Silva Carlos J.2ORCID,Geiger Johannes3,Plank Christian3ORCID,Evans Christopher H.1ORCID,Balmayor Elizabeth R.14ORCID

Affiliation:

1. Rehabilitation Medicine Research Center, Mayo Clinic, Rochester, MN, USA.

2. cBITE, MERLN Institute for Technology-Inspired Regenerative Medicine, Maastricht University, Maastricht, Netherlands.

3. Ethris GmbH, Planegg, Germany.

4. IBE, MERLN Institute for Technology-Inspired Regenerative Medicine, Maastricht University, Maastricht, Netherlands.

Abstract

Large segmental osseous defects heal poorly. Recombinant, human bone morphogenetic protein-2 (rhBMP-2) is used clinically to promote bone healing, but it is applied at very high doses that cause adverse side effects and raise costs while providing only incremental benefit. We describe a previously unexplored, alternative approach to bone regeneration using chemically modified messenger RNA (cmRNA). An optimized cmRNA encoding BMP-2 was delivered to critical-sized femoral osteotomies in rats. The cmRNA remained orthotopically localized and generated BMP locally for several days. Defects healed at doses ≥25 μg of BMP-2 cmRNA. By 4 weeks, all animals treated with 50 μg of BMP-2 cmRNA had bridged bone defects without forming the massive callus seen with rhBMP-2. Moreover, such defects recovered normal mechanical strength quicker and initiated bone remodeling faster. cmRNA regenerated bone via endochondral ossification, whereas rhBMP-2 drove intramembranous osteogenesis; cmRNA provides an innovative, safe, and highly translatable technology for bone healing.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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