首页> 外文期刊>European journal of human genetics: EJHG >Identification of a novel ARL13B variant in a Joubert syndrome-affected patient with retinal impairment and obesity
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Identification of a novel ARL13B variant in a Joubert syndrome-affected patient with retinal impairment and obesity

机译:乔伯特综合征视网膜病变和肥胖患者的新型ARL13B变种的鉴定。

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摘要

Joubert syndrome (JS) is a genetically heterogeneous autosomal recessive ciliopathy with 22 genes implicated to date, including a small, ciliary GTPase, ARL13B. ARL13B is required for cilia formation in vertebrates. JS patients display multiple symptoms characterized by ataxia due to the cerebellar vermis hypoplasia, and that can also include ocular abnormalities, renal cysts, liver fibrosis or polydactyly. These symptoms are shared with other ciliopathies, some of which display additional phenotypes, such as obesity. Here we identified a novel homozygous missense variant in ARL13B/JBTS8 in a JS patient who displayed retinal defects and obesity. We demonstrate the variant disrupts ARL13B function, as its expression did not rescue the mutant phenotype either in Arl13b(scorpion) zebrafish or in Arl13b(hennin) mouse embryonic fibroblasts, while the wild-type ARL13B did. Finally, we show that ARL13B is localized within the primary cilia of neonatal mouse hypothalamic neurons consistent with the known link between hypothalamic ciliary function and obesity. Thus our data identify a novel ARL13B variant that causes JS and retinopathy and suggest an extension of the phenotypic spectrum of ARL13B mutations to obesity.
机译:Joubert综合征(JS)是遗传异质性常染色体隐性纤毛病,迄今涉及22个基因,包括小型睫状GTPase ARL13B。脊椎动物纤毛形成需要ARL13B。 JS患者表现出多种症状,这些症状由于小脑ver部发育不全而导致共济失调,还可能包括眼部异常,肾囊肿,肝纤维化或多发性。这些症状与其他纤毛病共有,其中一些表现出其他表型,例如肥胖。在这里,我们在显示视网膜缺损和肥胖的JS患者中,在ARL13B / JBTS8中鉴定了一种新型的纯合错义变体。我们证明了该变体破坏了ARL13B的功能,因为其表达不能挽救Arl13b(蝎子)斑马鱼或Arl13b(hennin)小鼠胚胎成纤维细胞中的突变表型,而野生型ARL13B却可以。最后,我们显示ARL13B位于新生小鼠下丘脑神经元的原发纤毛内,与下丘脑睫状功能和肥胖之间的已知联系一致。因此,我们的数据确定了导致JS和视网膜病变的新型ARL13B变体,并暗示了ARL13B突变的表型谱向肥胖的延伸。

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