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卵泡抑素限制骨形态发生蛋白(BMP)-2对胎鼠下颌细胞中破骨细胞分化的作用。

Follistatin restricts bone morphogenetic protein (BMP)-2 action on the differentiation of osteoblasts in fetal rat mandibular cells.

作者信息

Abe Yukiko, Abe Tatsuya, Aida Yoshitomi, Hara Yoshitaka, Maeda Katsumasa

机构信息

Division of Periodontology, Department of Developmental and Reconstructive Medicine, Course of Medical and Dental Sciences, Nagasaki University Graduate School, Nagasaki, Japan.

出版信息

J Bone Miner Res. 2004 Aug;19(8):1302-7. doi: 10.1359/JBMR.040408. Epub 2004 May 3.

Abstract

UNLABELLED

We tested whether FS secretion might modulate BMP-2 actions by measuring FS levels and counting bone numbers of rat mandibular cells. In the presence of Dex, BMP-2 stimulated FS secretion at the early phase and augmented bone nodule by neutralizing with FS antibody. We concluded that BMP-2 facilitates FS secretion, and the FS restricts BMP-2 action on osteoblastogenesis.

INTRODUCTION

Bone morphogenetic proteins (BMPs) promote the differentiation of osteoprogenitor cells into osteoblasts. Activin A is involved in the regulation of bone formation. Follistatin (FS) antagonizes the bioactivities of BMP and activin A extracellularly.

MATERIALS AND METHODS

In this study, we tested whether the induction of FS secretion might modulate the effects of BMP-2 on osteoblast development, using the bone nodule-forming cultures of fetal rat mandibular cells.

RESULTS AND CONCLUSIONS

In the presence of dexamethasone (Dex), BMP-2 stimulated the secretion of FS at the early phase (days 3-9) of the culture. Dex alone had no effect, and BMP-2 alone was less effective than the combination of the two. BMP-4 and -6 had little effect on FS secretion. Activin A inhibited the early upregulation of FS secretion when added with BMP-2 and Dex. In the presence of Dex, BMP-2 increased bone nodule numbers when added to early cultures. The addition of anti-FS antibody to cultures with BMP-2 and Dex augmented bone nodule formation. These results show that BMP-2 facilitates the secretion of FS in the presence of Dex, and the increased FS secretion restricts the action of BMP-2 on osteoblast differentiation.

摘要

未标记

我们通过测量大鼠下颌细胞的卵泡抑素(FS)水平并计算骨数量,来测试FS分泌是否可能调节骨形态发生蛋白-2(BMP-2)的作用。在存在地塞米松(Dex)的情况下,BMP-2在早期刺激FS分泌,并通过用FS抗体中和来增加骨结节。我们得出结论,BMP-2促进FS分泌,并且FS限制BMP-2对成骨细胞生成的作用。

引言

骨形态发生蛋白(BMPs)促进骨祖细胞向成骨细胞分化。激活素A参与骨形成的调节。卵泡抑素(FS)在细胞外拮抗BMP和激活素A的生物活性。

材料与方法

在本研究中,我们使用胎鼠下颌细胞的骨结节形成培养物,测试FS分泌的诱导是否可能调节BMP-2对成骨细胞发育的影响。

结果与结论

在地塞米松(Dex)存在的情况下,BMP-2在培养的早期阶段(第3 - 9天)刺激FS分泌。单独的Dex没有作用,单独的BMP-2比两者组合的效果差。BMP-4和-6对FS分泌几乎没有影响。当与BMP-2和Dex一起添加时,激活素A抑制FS分泌的早期上调。在存在Dex的情况下,BMP-2添加到早期培养物中时增加了骨结节数量。向含有BMP-2和Dex的培养物中添加抗FS抗体增加了骨结节形成。这些结果表明,在存在Dex的情况下,BMP-2促进FS分泌,并且增加的FS分泌限制了BMP-2对成骨细胞分化的作用。

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