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Cell biology of osteochondromas: Bone morphogenic protein signalling and heparan sulphates

机译:骨软骨瘤的细胞生物学:骨形态发生蛋白信号传导和硫酸乙酰肝素

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Frequent benign outgrowths from bone known as osteochondromas, exhibiting typical endochondral ossification, are reported from single to multiple lesions. Characterised by a high incidence of osteochondromas and skeletal deformities, multiple hereditary exostoses (MHE) is the most common inherited musculoskeletal condition. While factors for severity remain unknown, mutations in exostosin 1 and exostosin 2 genes, encoding glycosyltransferases involved in the biosynthesis of ubiquitously expressed heparan sulphate (HS) chains, are associated with MHE. HS-binding bone morphogenetic proteins (BMPs) are multifunctional proteins involved in the morphogenesis of bone and cartilage. HS and HS proteoglycans are involved in BMP-mediated morphogenesis by regulating their gradient formation and activity. Mutations in exostosin genes disturb HS biosynthesis, subsequently affecting its functional role in the regulation of signalling pathways. As BMPs are the primordial morphogens for bone development, we propose the hypothesis that BMP signalling may be critical in osteochondromas. For this reason, the outcomes of exostosin mutations on HS biosynthesis and interactions within osteochondromas and MHE are reviewed. Since BMPs are HS binding proteins, the interactions of HS with the BMP signalling pathway are discussed. The impact of mouse models in the quest to better understand the cell biology of osteochondromas is discussed. Several challenges and questions still remain and further investigations are needed to explore new approaches for better understanding of the pathogenesis of osteochondromas.
机译:据报道,从单个病变到多个病变,经常发生的良性骨坏死(称为骨软骨瘤)表现出典型的软骨内骨化。多发性遗传性骨赘(MHE)以骨软骨瘤和骨骼畸形的高发为特征,是最常见的遗传性骨骼肌疾病。虽然严重性的因素仍然未知,但编码泛素表达的硫酸乙酰肝素(HS)链生物合成中涉及的糖基转移酶的外泌素1和外泌素2基因突变与MHE相关。 HS结合骨形态发生蛋白(BMP)是参与骨骼和软骨形态发生的多功能蛋白。 HS和HS蛋白聚糖通过调节其梯度形成和活性参与BMP介导的形态发生。外泌素基因的突变会干扰HS的生物合成,从而影响其在信号通路调控中的功能。由于BMP是骨骼发育的原始形态发生剂,因此我们提出了BMP信号可能在骨软骨瘤中起关键作用的假设。因此,综述了外泌素突变对HS生物合成的结果以及骨软骨瘤和MHE之间的相互作用。由于BMP是HS结合蛋白,因此将讨论HS与BMP信号通路的相互作用。为了更好地了解骨软骨瘤的细胞生物学,讨论了小鼠模型的影响。仍然存在一些挑战和问题,需要进一步研究以探索新方法,以更好地了解骨软骨瘤的发病机理。

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