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2例FAM20 A基因突变患者的釉质-肾综合征及非典型多毛症和听力损失表型

Enamel-renal syndrome in 2 patients with a mutation in FAM20 A and atypical hypertrichosis and hearing loss phenotypes.

作者信息

Pêgo Sabina Pena B, Coletta Ricardo D, Dumitriu Simona, Iancu Daniela, Albanyan Saleh, Kleta Robert, Auricchio Maria Teresa, Santos Luis Antônio, Rocha Breno, Martelli-Júnior Hercílio

机构信息

Stomatology Clinic, Dental School, State University of Montes Claros, Montes Claros, Minas Gerais, Brazil.

Department of Oral Diagnosis, School of Dentistry, University of Campinas, Piracicaba, São Paulo, Brazil.

出版信息

Oral Surg Oral Med Oral Pathol Oral Radiol. 2017 Feb;123(2):229-234.e2. doi: 10.1016/j.oooo.2016.09.226. Epub 2016 Oct 13.

Abstract

Enamel-renal syndrome (OMIM #204690) is an uncommon disorder characterized by amelogenesis imperfecta and nephrocalcinosis and is caused by mutations in FAM20 A. We report 2 patients with enamel-renal syndrome who exhibited the typical features of this syndrome and a homozygous nonsense mutation in the FAM20 A gene (c.406 C>T), genetically confirming the diagnosis. They also exhibited 2 undescribed clinical features, hypertrichosis and hearing loss. Alterations in genes frequently associated with nonsyndromic hearing loss in the Brazilian population, including connexin 26 (GJB2), connexin 30 (GJB6) and mitochondrial 12 S rRNA (m.A1555 G mutation), were not found. These results suggest a putative function of FAM20 A in the development of the inner ear and in the formation of hair. The presence of nephrocalcinosis is a risk factor for renal impairment, and it is important to perform regular renal monitoring in order to avoid renal failure.

摘要

釉质-肾综合征(OMIM #204690)是一种罕见的疾病,其特征为牙釉质发育不全和肾钙质沉着症,由FAM20 A基因突变引起。我们报告了2例釉质-肾综合征患者,他们表现出该综合征的典型特征,并且FAM20 A基因存在纯合无义突变(c.406 C>T),从基因层面证实了诊断。他们还表现出2种未被描述的临床特征,即多毛症和听力损失。在巴西人群中,未发现与非综合征性听力损失频繁相关的基因改变,包括连接蛋白26(GJB2)、连接蛋白30(GJB6)和线粒体12 S rRNA(m.A1555 G突变)。这些结果提示FAM20 A在内耳发育和毛发形成中可能具有某种功能。肾钙质沉着症的存在是肾功能损害的一个危险因素,定期进行肾脏监测以避免肾衰竭很重要。

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