Common skeletal features in rare diseases: New links between ciliopathies and FGF-related syndromes.

Rare diseases (Austin, Tex.) Pub Date : 2013-11-11 eCollection Date: 2013-01-01 DOI:10.4161/rdis.27109
Basil Z Yannakoudakis, Karen J Liu
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引用次数: 2

Abstract

Congenital skeletal anomalies are rare disorders, with a subset affecting both the cranial and appendicular skeleton. Two categories, craniosynostosis syndromes and chondrodysplasias, frequently result from aberrant regulation of the fibroblast growth factor (FGF) signaling pathway. Our recent work has implicated FGF signaling in a third category: ciliopathic skeletal dysplasias. In this work, we have used mouse mutants in two ciliopathy genes, Fuzzy (Fuz) and orofacial digital syndrome-1 (Ofd-1), to demonstrate increase in Fgf8 gene expression during critical stages of embryogenesis. While the mechanisms underlying FGF dysregulation differ in the different syndromes, our data raise the possibility that convergence on FGF signal transduction may underlie a wide range of skeletal anomalies. Here, we provide additional evidence of the skeletal phenotypes from the Fuz mouse model and highlight similarities between human ciliopathies and FGF-related syndromes.

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罕见疾病的常见骨骼特征:纤毛病与fgf相关综合征之间的新联系
先天性骨骼异常是罕见的疾病,影响颅骨和阑尾骨骼的一个子集。颅缝闭锁综合征和软骨发育不良通常是由成纤维细胞生长因子(FGF)信号通路的异常调节引起的。我们最近的工作暗示了FGF信号在第三类:纤毛性骨骼发育不良。在这项工作中,我们使用小鼠两种纤毛病基因的突变体,Fuzzy (Fuz)和orofacial digital syndrome-1 (Ofd-1),来证明Fgf8基因在胚胎发生的关键阶段表达增加。虽然FGF失调的机制在不同的综合征中有所不同,但我们的数据提出了FGF信号转导趋同可能是多种骨骼异常的基础。在这里,我们提供了来自Fuz小鼠模型的骨骼表型的额外证据,并强调了人类纤毛病和fgf相关综合征之间的相似性。
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