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首页> 外文期刊>European journal of oral sciences >Functional evaluation of a novel tooth agenesis-associated bone morphogenetic protein 4 prodomain mutation
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Functional evaluation of a novel tooth agenesis-associated bone morphogenetic protein 4 prodomain mutation

机译:新型牙齿发育不全相关骨形态发生蛋白4前结构域突变的功能评价

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摘要

The detection of gene mutations in patients with congenitally missing teeth is not very complicated; however, proving causality is often quite difficult. Here, we report the detection of a substitution mutation, A42P, within the prodomain of bone morphogenetic protein 4 (BMP4) in a small family with tooth agenesis and describe a functional alteration that may be responsible for the tooth phenotype. As BMP4 is essential for the development of teeth and also for many other organs, it would be of considerable interest to find a BMP4 mutation that is associated only with tooth agenesis. Our in vitro investigations revealed that the A42P mutation neither affected processing and secretion of BMP4 nor altered functional properties, such as the induction of alkaline phosphatase or signaling through Smad1/5/8 phosphorylation by the mature BMP4 ligand. However, immunofluorescence staining revealed that the prodomains of BMP4 which harbor the A42P substitution form fibrillar structures around transfected cells in culture and that this fibrillar network is significantly decreased when mutant prodomains are expressed. Our finding suggests that in vivo, BMP4 prodomain behavior might also be altered by the mutation and could influence storage or transport of mature BMP4 in the extracellular matrix of the developing tooth.
机译:先天性牙齿缺失患者的基因突变检测不是很复杂;但是,证明因果关系通常很困难。在这里,我们报告检测到的一个小家族中发生牙齿发育异常的骨形态发生蛋白4(BMP4)的前结构域中的替代突变A42P,并描述了可能导致牙齿表型的功能改变。由于BMP4对牙齿以及许多其他器官的发育至关重要,因此寻找仅与牙齿发育不全相关的BMP4突变将引起人们极大的兴趣。我们的体外研究表明,A42P突变既不会影响BMP4的加工和分泌,也不会改变功能特性,例如诱导碱性磷酸酶或通过成熟的BMP4配体通过Smad1 / 5/8磷酸化产生信号。但是,免疫荧光染色显示,带有A42P取代的BMP4的前结构域在培养的转染细胞周围形成了原纤维结构,当表达突变前结构域时,该原纤维网络显着减少。我们的发现表明,在体内,BMP4前结构域的行为也可能会因突变而改变,并可能影响成熟BMP4在发育中牙齿的细胞外基质中的储存或​​运输。

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