| Literature DB >> 24046454 |
Aline Bozec1, Latifa Bakiri, Maria Jimenez, Evan D Rosen, Philip Catalá-Lehnen, Thorsten Schinke, Georg Schett, Michael Amling, Erwin F Wagner.
Abstract
Recent studies have established that the skeleton functions as an endocrine organ affecting metabolism through the osteoblast-derived hormone osteocalcin (Ocn). However, it is not fully understood how many transcription factors expressed in osteoblasts regulate the endocrine function. Here, we show that mice with osteoblast-specific deletion of Fra-2 (Fosl2) have low bone mass but increased body weight. In contrast, transgenic expression of Fra-2 in osteoblasts leads to increased bone mass and decreased body weight accompanied by reduced serum glucose and insulin levels, improved glucose tolerance and insulin sensitivity. In addition, mice lacking Fra-2 have reduced levels of circulating Ocn, but high adiponectin (Adipoq), whereas Fra-2 transgenic mice exhibit high Ocn and low Adipoq levels. Moreover, we found that Adipoq was expressed in osteoblasts and that this expression was transcriptionally repressed by Fra-2. These results demonstrate that Fra-2 expression in osteoblasts represents a novel paradigm for a transcription factor controlling the endocrine function of the skeleton.Entities:
Keywords: AP-1; Activator protein 1; Adiponectin; Fosl2; Fra-2; Metabolism; Osteoblasts; Osteocalcin
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Year: 2013 PMID: 24046454 DOI: 10.1242/jcs.134510
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285