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软骨内骨化过程中信号素3A及其受体的表达:在骨骼发育和神经支配中的潜在作用

Expression of Semaphorin-3A and its receptors in endochondral ossification: potential role in skeletal development and innervation.

作者信息

Gomez C, Burt-Pichat B, Mallein-Gerin F, Merle B, Delmas P D, Skerry T M, Vico L, Malaval L, Chenu C

机构信息

INSERM, Unit 403, Lyon, France.

出版信息

Dev Dyn. 2005 Oct;234(2):393-403. doi: 10.1002/dvdy.20512.

Abstract

Bone tissue is densely innervated, and there is increasing evidence for a neural control of bone metabolism. Semaphorin-3A is a very important regulator of neuronal targeting in the peripheral nervous system as well as in angiogenesis, and knockout of the Semaphorin-3A gene induces abnormal bone and cartilage development. We analyzed the spatial and temporal expression patterns of Semaphorin-3A signaling molecules during endochondral ossification, in parallel with the establishment of innervation. We show that osteoblasts and chondrocytes differentiated in vitro express most members of the Semaphorin-3A signaling system (Semaphorin-3A, Neuropilin-1, and Plexins-A1 and -A2). In vitro, osteoclasts express most receptor chains but not the ligand. In situ, these molecules are all expressed in the periosteum and by resting, prehypertrophic and hypertrophic chondrocytes in ossification centers before the onset of neurovascular invasion. They are detected later in osteoblasts and also osteoclasts, with differences in intensity and regional distribution. Semaphorin-3A and Neuropilin-1 are also expressed in the bone marrow. Plexin-A3 is not expressed by bone cell lineages in vitro. It is detected early in the periosteum and hypertrophic chondrocytes. After the onset of ossification, this chain is restricted to a network of cell processes in close vicinity to the cells lining the trabeculae, similar to the pattern observed for neural markers at the same stages. After birth, while the density of innervation decreases, Plexin-A3 is strongly expressed by blood vessels on the ossification front. In conclusion, Semaphorin-3A signaling is present in bone and seems to precede or coincide at the temporal but also spatial level with the invasion of bone by blood vessels and nerve fibers. Expression patterns suggest Plexin-A3/Neuropilin-1 as a candidate receptor in target cells for the regulation of bone innervation by Semaphorin-3A.

摘要

骨组织神经分布密集,越来越多的证据表明存在对骨代谢的神经控制。信号素3A是外周神经系统以及血管生成中神经元靶向的非常重要的调节因子,信号素3A基因敲除会诱导骨骼和软骨发育异常。我们分析了软骨内成骨过程中信号素3A信号分子的时空表达模式,并与神经支配的建立同时进行。我们发现,体外分化的成骨细胞和软骨细胞表达信号素3A信号系统的大多数成员(信号素3A、神经纤毛蛋白-1以及丛状蛋白-A1和-A2)。在体外,破骨细胞表达大多数受体链,但不表达配体。在原位,这些分子均在骨膜以及神经血管侵入开始前的骨化中心的静止、前肥大和肥大软骨细胞中表达。随后在成骨细胞以及破骨细胞中也能检测到它们,强度和区域分布存在差异。信号素3A和神经纤毛蛋白-1也在骨髓中表达。丛状蛋白-A3在体外的骨细胞谱系中不表达。它在骨膜和肥大软骨细胞中早期被检测到。骨化开始后,这条链局限于靠近小梁内衬细胞的细胞突起网络中,类似于同一阶段神经标记物观察到的模式。出生后,虽然神经支配密度降低,但丛状蛋白-A3在骨化前沿的血管中强烈表达。总之,信号素3A信号存在于骨中,并且在时间和空间水平上似乎先于或与血管和神经纤维侵入骨同时发生。表达模式表明丛状蛋白-A3/神经纤毛蛋白-1是信号素3A调节骨神经支配的靶细胞中的候选受体。

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