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Ghrelin is an Osteoblast Mitogen and Increases Osteoclastic Bone Resorption In Vitro

机译:Ghrelin是成骨细胞的促分裂原,可增加体外破骨细胞的骨吸收。

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Ghrelin is released in response to fasting, such that circulating levels are highest immediately prior to meals. Bone turnover is acutely responsive to the fed state, with increased bone resorption during fasting and suppression during feeding. The current study investigated the hypothesis that ghrelin regulates the activity of bone cells. Ghrelin increased the bone-resorbing activity of rat osteoclasts, but did not alter osteoclast differentiation in a murine bone marrow assay nor bone resorption in ex vivo calvarial cultures. Ghrelin showed mitogenic activity in osteoblasts, with a strong effect in human cells and a weaker effect in rat osteoblasts. The expression of the human ghrelin receptor, GHSR, varied among individuals and was detectable in 25–30% of bone marrow and osteoblast samples. However, the rodentGhsrexpression was undetectable in bone cells and cell lines from rat and mouse. These data suggest that elevated levels of ghrelin may contribute to the higher levels of bone turnover that occurs in the fasted state.
机译:Ghrelin是根据禁食而释放的,因此就餐前的循环水平最高。骨转换对进食状态有敏锐反应,禁食期间骨骼吸收增加,进食期间受到抑制。当前的研究调查了生长素释放肽调节骨细胞活性的假说。 Ghrelin增加了大鼠破骨细胞的骨吸收活性,但是在鼠骨髓试验中没有改变破骨细胞的分化,也没有改变离体颅盖骨培养物中的骨吸收。 Ghrelin在成骨细胞中显示有丝分裂活性,对人细胞有强烈作用,而对大鼠成骨细胞则有较弱的作用。人类生长素释放肽受体GHSR的表达因个体而异,在25%至30%的骨髓和成骨细胞样本中可检测到。然而,在大鼠和小鼠的骨细胞和细胞系中,啮齿动物的Ghsrexpression无法检测到。这些数据表明,生长激素释放肽的水平升高可能导致禁食状态下发生的骨代谢水平升高。

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