首页> 美国卫生研究院文献>American Journal of Human Genetics >Homozygous Mutations in ADAMTS10 and ADAMTS17 Cause Lenticular Myopia Ectopia Lentis Glaucoma Spherophakia and Short Stature
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Homozygous Mutations in ADAMTS10 and ADAMTS17 Cause Lenticular Myopia Ectopia Lentis Glaucoma Spherophakia and Short Stature

机译:ADAMTS10和ADAMTS17中的纯合突变会导致晶状体近视埃塞俄比亚Lentis青光眼球状体和身材矮小

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摘要

Weill-Marchesani syndrome (WMS) is a well-characterized disorder in which patients develop eye and skeletal abnormalities. Autosomal-recessive and autosomal-dominant forms of WMS are caused by mutations in ADAMTS10 and FBN1 genes, respectively. Here we report on 13 patients from seven unrelated families from the Arabian Peninsula. These patients have a constellation of features that fall within the WMS spectrum and follow an autosomal-recessive mode of inheritance. Individuals who came from two families and met the diagnostic criteria for WMS were each found to have a different homozygous missense mutation in ADAMTS10. Linkage analysis and direct sequencing of candidate genes in another two families and a sporadic case with phenotypes best described as WMS-like led to the identification of three homozygous mutations in the closely related ADAMTS17 gene. Our clinical and genetic findings suggest that ADAMTS17 plays a role in crystalline lens zonules and connective tissue formation and that mutations in ADAMTS17 are sufficient to produce some of the main features typically described in WMS.
机译:Weill-Marchesani综合征(WMS)是一种特征鲜明的疾病,患者会出现眼部和骨骼异常。 WMS的常染色体隐性和常染色体显性形式分别由ADAMTS10和FBN1基因的突变引起。在这里,我们报告了来自阿拉伯半岛七个无关家庭的13名患者。这些患者的特征星座属于WMS谱,并遵循常染色体隐性遗传方式。来自两个家庭并符合WMS诊断标准的个体均被发现在ADAMTS10中具有不同的纯合错义突变。对另外两个家族中候选基因的连锁分析和直接测序,以及一个偶发性病例,其表型最能描述为WMS样,从而导致在密切相关的ADAMTS17基因中鉴定出三个纯合突变。我们的临床和遗传发现表明,ADAMTS17在晶状体小带和结缔组织形成中起作用,ADAMTS17中的突变足以产生WMS中通常描述的一些主要特征。

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