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首页> 外文OA文献 >Mutations in the DBP-Deficiency Protein HSD17B4 Cause Ovarian Dysgenesis, Hearing Loss, and Ataxia of Perrault Syndrome
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Mutations in the DBP-Deficiency Protein HSD17B4 Cause Ovarian Dysgenesis, Hearing Loss, and Ataxia of Perrault Syndrome

机译:DBP缺陷蛋白HSD17B4中的突变导致卵巢发育不全,听力丧失和Perrault综合征的共济失调

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Perrault syndrome is a recessive disorder characterized by ovarian dysgenesis in females, sensorineural deafness in both males and females, and in some patients, neurological manifestations. No genes for Perrault syndrome have heretofore been identified. A small family of mixed European ancestry includes two sisters with well-characterized Perrault syndrome. Whole-exome sequencing of genomic DNA from one of these sisters revealed exactly one gene with two rare functional variants: HSD17B4, which encodes 17β-hydroxysteroid dehydrogenase type 4 (HSD17B4), also known as D-bifunctional protein (DBP). HSD17B4/DBP is a multifunctional peroxisomal enzyme involved in fatty acid β-oxidation and steroid metabolism. Both sisters are compound heterozygotes for HSD17B4 c.650A>G (p.Y217C) (maternal allele) and HSB17B4 c.1704T>A (p.Y568X) (paternal allele). The missense mutation is predicted by structural analysis to destabilize the HSD17B4 dehydrogenase domain. The nonsense mutation leads to very low levels of HSD17B4 transcript. Expression of mutant HSD17B4 protein in a compound heterozygote was severely reduced. Mutations in HSD17B4 are known to cause DBP deficiency, an autosomal-recessive disorder of peroxisomal fatty acid β-oxidation that is generally fatal within the first two years of life. No females with DBP deficiency surviving past puberty have been reported, and ovarian dysgenesis has not previously been associated with this illness. Six other families with Perrault syndrome have wild-type sequences of HSD17B4. These results indicate that Perrault syndrome and DBP deficiency overlap clinically; that Perrault syndrome is genetically heterogeneous; that DBP deficiency may be underdiagnosed; and that whole-exome sequencing can reveal critical genes in small, nonconsanguineous families.
机译:Perrault综合征是一种隐性疾病,其特征是女性卵巢发育不全,男性和女性的感音神经性耳聋,以及某些患者的神经系统表现。迄今为止,尚未鉴定出Perrault综合征的基因。欧洲血统的一个小家庭包括两个患有特征性Perrault综合征的姐妹。这些姐妹之一的基因组DNA的全外显子测序揭示了一个具有两个罕见功能变体的基因:HSD17B4,其编码17β-羟基类固醇脱氢酶4型(HSD17B4),也称为D双功能蛋白(DBP)。 HSD17B4 / DBP是涉及脂肪酸β-氧化和类固醇代谢的多功能过氧化物酶体酶。两个姐妹都是HSD17B4 c.650A> G(p.Y217C)(母亲等位基因)和HSB17B4 c.1704T> A(p.Y568X)(父亲等位基因)的复合杂合子。通过结构分析预测错义突变使HSD17B4脱氢酶结构域不稳定。无意义的突变导致非常低水平的HSD17B4转录物。突变HSD17B4蛋白在复合杂合子中的表达大大降低。已知HSD17B4中的突变会导致DBP缺乏,这是一种过氧化物酶体脂肪酸β-氧化的常染色体隐性疾病,通常在生命的头两年内致命。尚无女性在青春期后幸存的DBP缺乏症的报道,并且卵巢发育不全以前与这种疾病无关。其他六个Perrault综合征家族具有HSD17B4的野生型序列。这些结果表明,Perrault综合征和DBP缺乏症在临床上有重叠。佩罗综合症在遗传上是异质的; DBP缺乏症可能被诊断不足;而且这种全外显子测序可以揭示小型,非近亲家庭中的关键基因。

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