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鉴定受体型蛋白酪氨酸磷酸酶μ作为骨细胞的新标志物。

Identification of receptor-type protein tyrosine phosphatase μ as a new marker for osteocytes.

作者信息

de Rooij Karien E, van der Velde Martijn, de Wilt Edwin, Deckers Martine M L, Bezemer Martineke, Waarsing Jan H, Que Ivo, Chan Alan B, Kaijzel Eric L, Löwik Clemens W G M

机构信息

Experimental Molecular Imaging, Department of Radiology, Leiden University Medical Center, Albinusdreef 2, PO Box 9600, 2300 RC, Leiden, The Netherlands,

出版信息

Histochem Cell Biol. 2015 Jul;144(1):1-11. doi: 10.1007/s00418-015-1319-1. Epub 2015 Apr 8.

Abstract

Osteocytes are the predominant cells in bone, where they form a cellular network and display important functions in bone homeostasis, phosphate metabolism and mechanical transduction. Several proteins strongly expressed by osteocytes are involved in these processes, e.g., sclerostin, DMP-1, PHEX, FGF23 and MEPE, while others are upregulated during differentiation of osteoblasts into osteocytes, e.g., osteocalcin and E11. The receptor-type protein tyrosine phosphatase µ (RPTPμ) has been described to be expressed in cells which display a cellular network, e.g., endothelial and neuronal cells, and is implied in mechanotransduction. In a capillary outgrowth assay using metatarsals derived from RPTPμ-knock-out/LacZ knock-in mice, we observed that the capillary structures grown out of the metatarsals were stained blue, as expected. Surprisingly, cells within the metatarsal bone tissue were positive for LacZ activity as well, indicating that RPTPμ is also expressed by osteocytes. Subsequent histochemical analysis showed that within bone, RPTPμ is expressed exclusively in early-stage osteocytes. Analysis of bone marrow cell cultures revealed that osteocytes are present in the nodules and an enzymatic assay enabled the quantification of the amount of osteocytes. No apparent bone phenotype was observed when tibiae of RPTPμ-knock-out/LacZ knock-in mice were analyzed by μCT at several time points during aging, although a significant reduction in cortical bone was observed in RPTPμ-knock-out/LacZ knock-in mice at 20 weeks. Changes in trabecular bone were more subtle. Our data show that RPTPμ is a new marker for osteocytes.

摘要

骨细胞是骨骼中的主要细胞,它们在其中形成细胞网络,并在骨稳态、磷酸盐代谢和机械转导中发挥重要作用。骨细胞强烈表达的几种蛋白质参与这些过程,例如骨硬化蛋白、牙本质基质蛋白-1(DMP-1)、磷酸调节中性肽酶(PHEX)、成纤维细胞生长因子23(FGF23)和基质细胞外磷糖蛋白(MEPE),而其他一些蛋白质在成骨细胞向骨细胞分化过程中上调,例如骨钙素和E11。据描述,受体型蛋白酪氨酸磷酸酶μ(RPTPμ)在具有细胞网络的细胞中表达,例如内皮细胞和神经元细胞,并参与机械转导。在使用源自RPTPμ基因敲除/ LacZ基因敲入小鼠的跖骨进行的毛细血管生长试验中,我们观察到从跖骨长出的毛细血管结构如预期那样被染成蓝色。令人惊讶的是,跖骨组织内的细胞LacZ活性也呈阳性,表明RPTPμ也由骨细胞表达。随后的组织化学分析表明,在骨内,RPTPμ仅在早期骨细胞中表达。对骨髓细胞培养物的分析表明,结节中存在骨细胞,并且酶促测定能够定量骨细胞的数量。在衰老过程中的几个时间点通过μCT分析RPTPμ基因敲除/ LacZ基因敲入小鼠的胫骨时,未观察到明显的骨表型,尽管在20周龄的RPTPμ基因敲除/ LacZ基因敲入小鼠中观察到皮质骨显著减少。小梁骨的变化更为细微。我们的数据表明,RPTPμ是骨细胞的一种新标志物。

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