首页> 外文期刊>The Journal of Steroid Biochemistry and Molecular Biology >Retinoic acid differentially affects in vitro proliferation, differentiation and mineralization of two fish bone-derived cell lines: Different gene expression of nuclear receptors and ECM proteins
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Retinoic acid differentially affects in vitro proliferation, differentiation and mineralization of two fish bone-derived cell lines: Different gene expression of nuclear receptors and ECM proteins

机译:视黄酸差异影响两种鱼骨来源细胞系的体外增殖,分化和矿化:核受体和ECM蛋白的基因表达不同

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Retinoic acid (RA), the main active metabolite of vitamin A, regulates vertebrate morphogenesis through signaling pathways not yet fully understood. Such process involves the specific activation of retinoic acid and retinoid X receptors (RARs and RXRs), which are nuclear receptors of the steroid/thyroid hormone receptor superfamily. Teleost fish are suitable models to study vertebrate development, such as skeletogenesis. Cell systems capable of in vitro mineralization have been developed for several fish species and may provide new insights into the specific cellular and molecular events related to vitamin A activity in bone, complementary to in vivo studies. This work aims at investigating the in vitro effects of RA (0.5 and 12.5 μM) on proliferation, differentiation and extracellular matrix (ECM) mineralization of two gilthead seabream bone-derived cell lines (VSa13 and VSa16), and at identifying molecular targets of its action through gene expression analysis. RA induced phenotypic changes and cellular proliferation was inhibited in both cell lines in a cell type-dependent manner (36-59% in VSa13 and 17-46% in VSa16 cells). While RA stimulated mineral deposition in VSa13 cell cultures (50-62% stimulation), it inhibited the mineralization of extracellular matrix in VSa16 cells (11-57% inhibition). Expression of hormone receptor genes (rars and rxrs), and extracellular matrix-related genes such as matrix and bone Gla proteins (mgp and bglap), osteopontin (spp1) and type I collagen (col1a1) were differentially regulated upon exposure to RA in proliferating, differentiating and mineralizing cultures of VSa13 and VSa16 cells. Altogether, our results show: (i) RA affects proliferative and mineralogenic activities in two fish skeletal cell types and (ii) that during phenotype transitions, specific RA nuclear receptors and bone-related genes are differentially expressed in a cell type-dependent manner.
机译:维甲酸(RA)是维生素A的主要活性代谢产物,它通过尚未完全了解的信号传导途径调节脊椎动物的形态发生。这种过程涉及视黄酸和类维生素A X受体(RAR和RXR)的特异性活化,这是类固醇/甲状腺激素受体超家族的核受体。硬骨鱼类是研究脊椎动物发育(例如骨骼形成)的合适模型。已经为几种鱼类开发了能够体外矿化的细胞系统,并且可以提供与体内研究相辅相成的与骨骼中维生素A活性有关的特定细胞和分子事件的新见解。这项工作旨在研究RA(0.5和12.5μM)对两种金头鲷鲷骨源性细胞系(VSa13和VSa16)增殖,分化和细胞外基质(ECM)矿化的体外影响,并确定其分子靶标通过基因表达分析来发挥作用。在两种细胞系中,RA诱导的表型变化和细胞增殖均以细胞类型依赖性方式受到抑制(VSa13中为36-59%,VSa16细胞为17-46%)。当RA刺激VSa13细胞培养物中的矿物质沉积(刺激50-62%)时,它抑制了VSa16细胞中细胞外基质的矿化(抑制11-57%)。激素受体基因(rars和rxrs)的表达以及细胞外基质相关基因(例如基质和骨Gla蛋白(mgp和bglap),骨桥蛋白(spp1)和I型胶原蛋白(col1a1)的表达在暴露于RA中均受到差异调节,分化和矿化VSa13和VSa16细胞。总而言之,我们的结果表明:(i)RA影响两种鱼类骨骼细胞类型的增殖和矿产活动,(ii)在表型过渡期间,特定的RA核受体和骨相关基因以细胞类型依赖性方式差异表达。

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