Vitamin-D Binding Protein Does Not Enhance Healing in Rat Bone Defects: A Pilot Study

Sun, Jui Sheng; Chen, Pei-Yu; Tsuang, Yang Hwei; Chen, Ming Hong; Chen, Po Quang

doi:10.1007/s11999-009-0864-0

Cited by 12 publications

(17 citation statements)

References 21 publications

(36 reference statements)

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“…Administration of a synthetic peptide fragment (consisting of 14 amino acids) derived from the human amino acid sequence at the site of glycosylation in the third domain of native DBP, to newborn rats (0.4 ng/g body weight) resulted in osteoinduction of the marrow cavity and osteogenesis of surrounding cortical and metaphyseal bone [116]. Those results could not be confirmed in an in vivo critical bone defect model, investigating the bone healing capacity of DBP [117]. However this study had several limitations.…”

Section: The Influence Of Vitamin D Binding Protein On T Cell Responsementioning

confidence: 96%

Behind the scenes of vitamin D binding protein: More than vitamin D binding

Delanghe

Speeckaert

2015

Best Practice & Research Clinical Endocrinology & Metab

139

122

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Section: The Influence Of Vitamin D Binding Protein On T Cell Responsementioning

confidence: 96%

Behind the scenes of vitamin D binding protein: More than vitamin D binding

Delanghe

Speeckaert

2015

Best Practice & Research Clinical Endocrinology & Metab

139

122

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“…Bone graft materials are often required for the treatment of large bone defects 40, 41. Producing appropriate bioactive bone graft materials for bone regeneration is a crucial issue in orthopedics.…”

Section: Discussionmentioning

confidence: 99%

Overexpression of Insulin-Like Growth Factor 1 Enhanced the Osteogenic Capability of Aging Bone Marrow Mesenchymal Stem Cells

et al. 2017

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Many studies have indicated that loss of the osteoblastogenic potential in bone marrow mesenchymal stem cells (bmMSCs) is the major component in the etiology of the aging-related bone deficit. But how the bmMSCs lose osteogenic capability in aging is unclear. Using 2-dimentional cultures, we examined the dose response of human bmMSCs, isolated from adult and aged donors, to exogenous insulin-like growth factor 1 (IGF-1), a growth factor regulating bone formation. The data showed that the mitogenic activity and the osteoblastogenic potential of bmMSCs in response to IGF-1 were impaired with aging, whereas higher doses of IGF-1 increased the proliferation rate and osteogenic potential of aging bmMSCs. Subsequently, we seeded IGF-1-overexpressing aging bmMSCs into calcium-alginate scaffolds and incubated in a bioreactor with constant perfusion for varying time periods to examine the effect of IGF-1 overexpression to the bone-forming capability of aging bmMSCs. We found that IGF-1 overexpression in aging bmMSCs facilitated the formation of cell clusters in scaffolds, increased the cell survival inside the cell clusters, induced the expression of osteoblast markers, and enhanced the biomineralization of cell clusters. These results indicated that IGF-1 overexpression enhanced cells' osteogenic capability. Thus, our data suggest that the aging-related loss of osteogenic potential in bmMSCs can be attributed in part to the impairment in bmMSCs' IGF-1 signaling, and support possible application of IGF-1-overexpressing autologous bmMSCs in repairing bone defect of the elderly and in producing bone graft materials for repairing large scale bone injury in the elderly.

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“…Recent development in tissue regeneration provided biomaterials for slow release of proteins over a period of time, thus giving cells continuous stimuli to differentiate into desired cells [60,65,66,68,70,73,75,76,78,92,[98][99][100]109,[116][117][118][119][120][121]. The level of gene expression in the surrounding tissue to regenerate bone can be enhanced by delivery of plasmid DNA using hydrogel microspheres, more than plasmid DNA solution.…”

Section: Discussionmentioning

confidence: 99%

“…The level of gene expression in the surrounding tissue to regenerate bone can be enhanced by delivery of plasmid DNA using hydrogel microspheres, more than plasmid DNA solution. BMP 2 -incorporated gelatin/ β-TCP scaffolds lead to significantly increased osteogenesis compared to the chem- ical induced osteogenesis in specimens [60,65,66,68,70,75,76,78,92,[98][99][100]109,[116][117][118][119][120][121]. In previous studies, various groups showed a continuous release of BMP2 in vitro and in vivo [65,66,68,70,73,75,76,92,[98][99][100]109,[119][120][121].…”

Section: Discussionmentioning

confidence: 99%