VEGF-C promotes the development of lymphatics in bone and bone loss.
Devon HominickAsitha SilvaNoor KhuranaYing LiuPaul C DechowJian Q FengBronislaw PytowskiJoseph M RutkowskiKari AlitaloMichael T DellingerPublished in: eLife (2018)
Patients with Gorham-Stout disease (GSD) have lymphatic vessels in their bones and their bones gradually disappear. Here, we report that mice that overexpress VEGF-C in bone exhibit a phenotype that resembles GSD. To drive VEGF-C expression in bone, we generated Osx-tTA;TetO-Vegfc double-transgenic mice. In contrast to Osx-tTA mice, Osx-tTA;TetO-Vegfc mice developed lymphatics in their bones. We found that inhibition of VEGFR3, but not VEGFR2, prevented the formation of bone lymphatics in Osx-tTA;TetO-Vegfc mice. Radiological and histological analysis revealed that bones from Osx-tTA;TetO-Vegfc mice were more porous and had more osteoclasts than bones from Osx-tTA mice. Importantly, we found that bone loss in Osx-tTA;TetO-Vegfc mice could be attenuated by an osteoclast inhibitor. We also discovered that the mutant phenotype of Osx-tTA;TetO-Vegfc mice could be reversed by inhibiting the expression of VEGF-C. Taken together, our results indicate that expression of VEGF-C in bone is sufficient to induce the pathologic hallmarks of GSD in mice.
Keyphrases
- bone loss
- high fat diet induced
- vascular endothelial growth factor
- endothelial cells
- bone mineral density
- wild type
- type diabetes
- lymph node
- metabolic syndrome
- computed tomography
- neoadjuvant chemotherapy
- skeletal muscle
- body composition
- postmenopausal women
- radiation therapy
- binding protein
- highly efficient
- locally advanced
- contrast enhanced