Literature DB >> 16145665

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

C Gomez1, B Burt-Pichat, F Mallein-Gerin, B Merle, P D Delmas, T M Skerry, L Vico, L Malaval, C Chenu.   

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. (c) 2005 Wiley-Liss, Inc.

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Year:  2005        PMID: 16145665     DOI: 10.1002/dvdy.20512

Source DB:  PubMed          Journal:  Dev Dyn        ISSN: 1058-8388            Impact factor:   3.780


  40 in total

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Review 3.  Plexin structures are coming: opportunities for multilevel investigations of semaphorin guidance receptors, their cell signaling mechanisms, and functions.

Authors:  Prasanta K Hota; Matthias Buck
Journal:  Cell Mol Life Sci       Date:  2012-06-29       Impact factor: 9.261

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Review 5.  Regulation of bone remodeling by the central and peripheral nervous system.

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Review 6.  Semaphorin 3A: A new player in bone remodeling.

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7.  Adenosine A2A receptor (A2AR) stimulation modulates expression of semaphorins 4D and 3A, regulators of bone homeostasis.

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8.  PLXNA2 identified as a candidate gene by genome-wide association analysis for mandibular prognathism in human chondrocytes.

Authors:  Takashi S Kajii; Akira Oka; Mitsutoki Hatta; Jun Yamazaki; Junro Yamashita; Junichiro Iida
Journal:  Biomed Rep       Date:  2018-07-11

9.  Semaphorin 3A promotes osteogenic differentiation in human alveolar bone marrow mesenchymal stem cells.

Authors:  Li Liu; Jue Wang; Xiaomeng Song; Qingping Zhu; Shuping Shen; Wei Zhang
Journal:  Exp Ther Med       Date:  2018-01-30       Impact factor: 2.447

10.  Tie2Cre-mediated inactivation of plexinD1 results in congenital heart, vascular and skeletal defects.

Authors:  Ying Zhang; Manvendra K Singh; Karl R Degenhardt; Min Min Lu; Jean Bennett; Yutaka Yoshida; Jonathan A Epstein
Journal:  Dev Biol       Date:  2008-10-17       Impact factor: 3.582

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