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首页> 外文期刊>The Journal of investigative dermatology. >RSPO4 is the major gene in autosomal-recessive anonychia and mutations cluster in the furin-like cysteine-rich domains of the Wnt signaling ligand R-spondin 4.
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RSPO4 is the major gene in autosomal-recessive anonychia and mutations cluster in the furin-like cysteine-rich domains of the Wnt signaling ligand R-spondin 4.

机译:RSPO4是常染色体隐性隐匿性甲虫的主要基因,其突变簇聚集在Wnt信号配体R-spondin 4的富弗林样富含半胱氨酸的域中。

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摘要

Congenital anonychia is a rare autosomal-recessive disorder characterized by the absence of finger- and toenails. Recently, we and others identified the secreted Wnt signaling ligand R-spondin 4 (RSPO4) as the first gene known to be responsible for inherited anonychia. R-spondins are secreted proteins that activate the Wnt/beta-catenin signaling pathway. This puts anonychia on the growing list of congenital malformation syndromes caused by Wnt signaling pathway defects. Here, we expand the RSPO4 mutational spectrum by identification of the previously unknown mutations c.190C>T (p.Arg64Cys) in exon 2 and c.301C>T (p.Gln101X) in exon 3, thereby corroborating R-spondin 4 as the major protein in autosomal-recessive anonychia. Almost all RSPO4 mutations detected so far affect the highly conserved exons 2 and 3. Thus, we postulate that RSPO4 mutations preferentially cluster in the furin-like cysteine-rich domains of R-spondin 4, which is in line with experimental data proposing that for beta-catenin stabilization, a shortened protein comprising just these two regions is sufficient.
机译:先天性甲沟炎是一种罕见的常染色体隐性遗传疾病,其特征是没有手指和脚趾甲。最近,我们和其他人将分泌的Wnt信号配体R-spondin 4(RSPO4)确定为已知负责遗传性甲虫的第一个基因。 R-spondins是激活Wnt /β-catenin信号通路的分泌蛋白。这使甲癣在由Wnt信号通路缺陷引起的先天性畸形综合症的清单上不断增加。在这里,我们通过鉴定外显子2中先前未知的突变c.190C> T(p.Arg64Cys)和外显子3中c.301C> T(p.Gln101X)来扩展RSPO4突变谱,从而证实R-spondin 4为常染色体隐性甲虫中的主要蛋白质。到目前为止,几乎所有检测到的RSPO4突变都会影响高度保守的外显子2和3。因此,我们推测RSPO4突变优先聚集在R-spondin 4富含弗林蛋白酶的半胱氨酸结构域中,这与实验数据相符。 β-catenin稳定,仅包含这两个区域的缩短蛋白就足够了。

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