| Literature DB >> 28972540 |
Omar Al Rifai1,2, Jacqueline Chow1, Julie Lacombe1, Catherine Julien1, Denis Faubert3, Delia Susan-Resiga4, Rachid Essalmani4, John Wm Creemers5, Nabil G Seidah4,6,7, Mathieu Ferron1,2,6,7.
Abstract
Osteocalcin (OCN) is an osteoblast-derived hormone that increases energy expenditure, insulin sensitivity, insulin secretion, and glucose tolerance. The cDNA sequence of OCN predicts that, like many other peptide hormones, OCN is first synthesized as a prohormone (pro-OCN). The importance of pro-OCN maturation in regulating OCN and the identity of the endopeptidase responsible for pro-OCN cleavage in osteoblasts are still unknown. Here, we show that the proprotein convertase furin is responsible for pro-OCN maturation in vitro and in vivo. Using pharmacological and genetic experiments, we also determined that furin-mediated pro-OCN cleavage occurred independently of its γ-carboxylation, a posttranslational modification that is known to hamper OCN endocrine action. However, because pro-OCN is not efficiently decarboxylated and activated during bone resorption, inactivation of furin in osteoblasts in mice resulted in decreased circulating levels of undercarboxylated OCN, impaired glucose tolerance, and reduced energy expenditure. Furthermore, we show that Furin deletion in osteoblasts reduced appetite, a function not modulated by OCN, thus suggesting that osteoblasts may secrete additional hormones that regulate different aspects of energy metabolism. Accordingly, the metabolic defects of the mice lacking furin in osteoblasts became more apparent under pair-feeding conditions. These findings identify furin as an important regulator of bone endocrine function.Entities:
Mesh:
Substances:
Year: 2017 PMID: 28972540 PMCID: PMC5663350 DOI: 10.1172/JCI93437
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808