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成骨细胞:骨组织中被忽视的一面。

Osteocyte: the unrecognized side of bone tissue.

机构信息

INSERM Research Unit 658, Centre Hospitalier Régional, 1 rue Porte Madeleine, 45 032 Orleans, France.

出版信息

Osteoporos Int. 2010 Sep;21(9):1457-69. doi: 10.1007/s00198-010-1194-5. Epub 2010 Mar 4.

Abstract

INTRODUCTION

Osteocytes represent 95% of all bone cells. These cells are old osteoblasts that occupy the lacunar space and are surrounded by the bone matrix. They possess cytoplasmic dendrites that form a canalicular network for communication between osteocytes and the bone surface. They express some biomarkers (osteopontin, beta3 integrin, CD44, dentin matrix protein 1, sclerostin, phosphate-regulating gene with homologies to endopeptidases on the X chromosome, matrix extracellular phosphoglycoprotein, or E11/gp38) and have a mechano-sensing role that is dependent upon the frequency, intensity, and duration of strain.

DISCUSSION

The mechanical information transmitted into the cytoplasm also triggers a biological cascade, starting with NO and PGE(2) and followed by Wnt/beta catenin signaling. This information is transmitted to the bone surface through the canalicular network, particularly to the lining cells, and is able to trigger bone remodeling by directing the osteoblast activity and the osteoclastic resorption. Furthermore, the osteocyte death seems to play also an important role. The outcome of micro-cracks in the vicinity of osteocytes may interrupt the canalicular network and trigger cell apoptosis in the immediate surrounding environment. This apoptosis appears to transmit a message to the bone surface and activate remodeling. The osteocyte network also plays a recognized endocrine role, particularly concerning phosphate regulation and vitamin D metabolism. Both the suppression of estrogen following menopause and chronic use of systemic glucocorticoids induce osteocyte apoptosis. On the other hand, physical activity has a positive impact in the reduction of apoptosis. In addition, some osteocyte molecular elements like sclerostin, connexin 43, E11/gp38, and DKK1 are emerging as promising targets for the treatment of various osteo-articular pathologies.

摘要

简介

骨细胞占所有骨细胞的 95%。这些细胞是旧的成骨细胞,它们占据了腔隙空间,并被骨基质包围。它们拥有细胞质树突,形成了一个骨细胞和骨表面之间的连通小管网。它们表达一些生物标志物(骨桥蛋白、β3 整合素、CD44、牙本质基质蛋白 1、硬骨素、具有 X 染色体内肽酶同源性的磷酸调节基因、细胞外基质磷酸糖蛋白或 E11/gp38),具有机械感受作用,该作用取决于应变的频率、强度和持续时间。

讨论

传入细胞质的机械信息也会引发一个生物级联反应,从 NO 和 PGE(2)开始,然后是 Wnt/β连环蛋白信号。这些信息通过连通小管网传递到骨表面,特别是传递到衬里细胞,并通过指导成骨细胞活性和破骨细胞吸收来触发骨重建。此外,骨细胞死亡似乎也起着重要作用。骨细胞附近微裂缝的结果可能会中断连通小管网,并触发周围环境中的细胞凋亡。这种凋亡似乎会向骨表面传递信息并激活重塑。骨细胞网络还具有公认的内分泌作用,特别是在调节磷酸盐和维生素 D 代谢方面。绝经后雌激素的抑制和长期使用全身糖皮质激素都会诱导骨细胞凋亡。另一方面,身体活动对减少凋亡有积极影响。此外,一些骨细胞分子元素,如硬骨素、连接蛋白 43、E11/gp38 和 DKK1,正作为治疗各种骨关节炎疾病的有前途的靶点出现。

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