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Osterix‐mCherry Expression Allows for Early Bone Detection in a Calvarial Defect Model
Author(s) -
Strecker Sara E.,
Unterman Shimon,
Charles Lyndon F.,
Pivovarchick Dmitry,
Maye Peter F.,
Edelman Elazer R.,
Artzi Natalie
Publication year - 2019
Publication title -
advanced biosystems
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.153
H-Index - 18
ISSN - 2366-7478
DOI - 10.1002/adbi.201900184
Subject(s) - chemistry , mcherry , microbiology and biotechnology , mesenchymal stem cell , biomedical engineering , bone formation , bone morphogenetic protein 2 , human bone , green fluorescent protein , gene , biology , endocrinology , in vitro , biochemistry , medicine
The process of new bone formation following trauma requires the temporal recruitment of cells to the site, including mesenchymal stem cells, preosteoblasts, and osteoblasts, the latter of which deposit minerals. Hence, bone repair, a process that is assessed by the extent of mineralization within the defect, can take months before it is possible to determine if a treatment is successful. Here, a fluorescently tagged Osterix, an early key gene in the bone formation cascade, is used as a predictive measure of bone formation. Using a calvarial defect model in mice, the ability to noninvasively track the Osterix transcription factor in an Osterix‐mCherry mouse model is evaluated as a measure for bone formation following treatment with recombinant human Bone‐Morphogenetic‐Protein 2 (rhBMP‐2). Two distinct delivery materials are utilized, an injectable nanocomposite hydrogel and a collagen sponge, that afford distinct release kinetics and it is found that cherry‐fluorescent protein can be detected as early as 2 weeks following treatment. Osterix intensity correlates with subsequent bone formation and hence can serve as a rapid screening tool for osteogenic drugs or for the evaluation and optimization of delivery platforms.

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