| Literature DB >> 32360587 |
Brianna H Shares1, Charles O Smith1, Tzong-Jen Sheu1, Rubens Sautchuk1, Kevin Schilling2, Laura C Shum1, Ananta Paine1, Aric Huber1, Emma Gira1, Edward Brown3, Hani Awad2, Roman A Eliseev4.
Abstract
Bone fracture is accompanied by trauma, mechanical stresses, and inflammation - conditions known to induce the mitochondrial permeability transition. This phenomenon occurs due to opening of the mitochondrial permeability transition pore (MPTP) promoted by cyclophilin D (CypD). MPTP opening leads to more inflammation, cell death and potentially to disruption of fracture repair. Here we performed a proof-of-concept study and tested a hypothesis that protecting mitochondria from MPTP opening via inhibition of CypD improves fracture repair. First, our in vitro experiments indicated pro-osteogenic and anti-inflammatory effects in osteoprogenitors upon CypD knock-out or pharmacological inhibition. Using a bone fracture model in mice, we observed that bone formation and biomechanical properties of repaired bones were significantly increased in CypD knock-out mice or wild type mice treated with a CypD inhibitor, NIM811, when compared to controls. These effects were evident in young male but not female mice, however in older (13 month-old) female mice bone formation was also increased during fracture repair. In contrast to global CypD knock-out, mesenchymal lineage-specific (Prx1-Cre driven) CypD deletion did not result in improved fracture repair. Our findings implicate MPTP in bone fracture and suggest systemic CypD inhibition as a modality to promote fracture repair.Entities:
Keywords: Bone fracture; Cyclophilin D; Mitochondria; Osteoprogenitors; Permeability transition
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Year: 2020 PMID: 32360587 PMCID: PMC7354230 DOI: 10.1016/j.bone.2020.115391
Source DB: PubMed Journal: Bone ISSN: 1873-2763 Impact factor: 4.398