Fam3c调节成骨细胞分化,影响骨体积和皮质骨矿物质密度。

BoneKEy reports Pub Date : 2016-04-06 eCollection Date: 2016-01-01 DOI:10.1038/bonekey.2016.14
Jorma A Määttä, Ameya Bendre, Mervi Laanti, Kalman G Büki, Pia Rantakari, Päivi Tervola, Johanna Saarimäki, Matti Poutanen, Pirkko Härkönen, Kalervo Väänänen
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引用次数: 19

摘要

Fam3c是一种细胞因子样生长因子,被认为在上皮-间质转化(EMT)、肿瘤生长和转移中起作用。在一项分析亚洲人群队列的研究中,在Fam3c基因的第一个内含子中发现了影响骨矿物质密度的单核苷酸多态性。其他针对不同人群的独立研究发现fam3c位点与骨密度和骨折有关。为了研究Fam3c在骨生物学中的作用,我们产生了Fam3c敲除(KO)小鼠品系。Fam3c KO小鼠外观、行为和生育能力正常,但骨骼形态和含量也有微小变化。雌性小鼠胫骨微ct分析显示小梁数量减少。在雄性小鼠中,骨表型变化较小,但观察到血液学变化。此外,雄性KO小鼠的体重与胫骨小梁和皮质骨体积呈负相关。皮质骨矿物质密度略有增加,但胫骨外侧断裂强度降低。Fam3c KO骨髓细胞在体外表现出加速的成骨分化和矿化。Fam3c小鼠骨小梁数量的减少和成骨分化的刺激表明Fam3c在成骨细胞分化和骨稳态中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Fam3c modulates osteogenic cell differentiation and affects bone volume and cortical bone mineral density.

Fam3c modulates osteogenic cell differentiation and affects bone volume and cortical bone mineral density.

Fam3c modulates osteogenic cell differentiation and affects bone volume and cortical bone mineral density.

Fam3c, a cytokine-like growth factor, has been suggested to have a role in epithelial-to-mesenchymal transition (EMT), tumor growth and metastasis. A single-nucleotide polymorphism affecting bone mineral density has been found in the first intron of the Fam3c gene in a study analyzing an Asian population cohort. Other independent studies on different population cohorts have found the fam3c locus to be associated with bone mineral density and fractures. In order to investigate the role of Fam3c in bone biology, we have generated a Fam3c knock-out (KO) mouse strain. The Fam3c KO mice were found to have normal appearance, behavior and fertility, but small changes in bone morphology and content were also observed. Micro-CT analysis of tibiae of the female mice revealed decreased number of trabeculae. In male mice the changes in the bone phenotype were smaller, but hematological changes were observed. Furthermore, there was a negative correlation between body weight and tibial trabecular and cortical bone volume in the male KO mice. There was a small increase in cortical bone mineral density, but in the lateral direction of tibiae the breaking strength was reduced. Fam3c KO bone marrow cells showed accelerated osteogenic differentiation and mineralization in vitro. The reduced number of bone trabeculae in Fam3c KO mice and the stimulated osteogenic differentiation indicate a role for Fam3c in osteoblast differentiation and bone homeostasis.

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