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矿化基质中的硬化蛋白与范布赫姆病

Sclerostin in mineralized matrices and van Buchem disease.

作者信息

van Bezooijen R L, Bronckers A L, Gortzak R A, Hogendoorn P C W, van der Wee-Pals L, Balemans W, Oostenbroek H J, Van Hul W, Hamersma H, Dikkers F G, Hamdy N A T, Papapoulos S E, Löwik C W G M

机构信息

Departments of Endocrinology and Metabolic Diseases, C4R, Leiden University Medical Center, Albinusdreef 2, Leiden 2333 ZA, The Netherlands.

出版信息

J Dent Res. 2009 Jun;88(6):569-74. doi: 10.1177/0022034509338340.

Abstract

Sclerostin is an inhibitor of bone formation expressed by osteocytes. We hypothesized that sclerostin is expressed by cells of the same origin and also embedded within mineralized matrices. In this study, we analyzed (a) sclerostin expression using immunohistochemistry, (b) whether the genomic defect in individuals with van Buchem disease (VBD) was associated with the absence of sclerostin expression, and (c) whether this was associated with hypercementosis. Sclerostin was expressed by cementocytes in mouse and human teeth and by mineralized hypertrophic chondrocytes in the human growth plate. In individuals with VBD, sclerostin expression was absent or strongly decreased in osteocytes and cementocytes. This was associated with increased bone formation, but no overt changes in cementum thickness. In conclusion, sclerostin is expressed by all 3 terminally differentiated cell types embedded within mineralized matrices: osteocytes, cementocytes, and hypertrophic chondrocytes.

摘要

硬化蛋白是一种由骨细胞表达的骨形成抑制剂。我们推测硬化蛋白由同源细胞表达,并且也嵌入矿化基质中。在本研究中,我们分析了:(a)使用免疫组织化学分析硬化蛋白表达;(b)范布赫姆病(VBD)患者的基因缺陷是否与硬化蛋白表达缺失有关;以及(c)这是否与牙骨质增生有关。硬化蛋白在小鼠和人类牙齿的牙骨质细胞以及人类生长板的矿化肥大软骨细胞中表达。在VBD患者中,骨细胞和牙骨质细胞中硬化蛋白表达缺失或显著降低。这与骨形成增加有关,但牙骨质厚度无明显变化。总之,硬化蛋白由嵌入矿化基质中的所有3种终末分化细胞类型表达:骨细胞、牙骨质细胞和肥大软骨细胞。

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