Androgen Insensitivity Syndrome DUE to Non-Coding Variation in the Androgen Receptor Gene: Review of the Literature and Case Report of a Patient with Mosaic c.-547C>T Variant.

IF 0.5 4区 医学 Q4 GENETICS & HEREDITY
P Noveski, T Plaseski, M Dimitrovska, D Plaseska-Karanfilska
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引用次数: 0

Abstract

Sexual development (SD) is a complex process with strict spatiotemporal regulation of gene expression. Despite advancements in molecular diagnostics, disorders of sexual development (DSD) have a diagnostic rate of ~50%. Androgen insensitivity syndrome (AIS) represents the most common form of 46,XY DSD, with a spectrum of defects in androgen action. Considering the importance of very strict regulation of the SD, it is reasonable to assume that the genetic cause for proportion of the DSD lies in the non-coding part of the genome that regulates proper gene functioning. Here we present a patient with partial AIS (PAIS) due to a mosaic de novo c.-547C>T pathogenic variant in the 5'UTR of androgen receptor (AR) gene. The same mutation was previously described as inherited, in two unrelated patients with complete AIS (CAIS). Thus, our case further confirms the previous findings that variable gene expressivity could be attributed to mosaicism. Mutations in 5'UTR could create new upstream open reading frames (uORFs) or could disrupt the existing one. A recent systematic genome-wide study identified AR as a member of a subset of genes where modifications of uORFs represents an important disease mechanism. Only a small number of studies are reporting non-coding mutations in the AR gene and our case emphasizes the importance of molecular testing of the entire AR locus in AIS patients. The introduction of new methods for comprehensive molecular testing in routine genetic diagnosis, accompanied with new tools for in sillico analysis could improve the genetic diagnosis of AIS, and DSD in general.

Abstract Image

雄激素受体基因非编码变异引起的雄激素不敏感综合征:文献综述及一例Mosaic c - 547c >T变异患者的病例报告
性发育是一个复杂的过程,具有严格的基因表达时空调控。尽管分子诊断技术取得了进步,但性发育障碍(DSD)的诊断率约为50%。雄激素不敏感综合征(AIS)是46xy DSD最常见的形式,具有雄激素作用的一系列缺陷。考虑到非常严格的SD调控的重要性,我们有理由认为DSD比例的遗传原因在于基因组中调控基因正常功能的非编码部分。在这里,我们报告了一例由于雄激素受体(AR)基因5'UTR中的c - 547c >T嵌合新发致病性变异而导致的部分AIS (PAIS)患者。相同的突变先前被描述为遗传性的,在两名无关的完全AIS (CAIS)患者中。因此,我们的病例进一步证实了先前的发现,即可变的基因表达可能归因于镶嵌现象。5'UTR的突变可能会产生新的上游开放阅读帧(uorf),也可能会破坏现有的uorf。最近一项系统的全基因组研究发现AR是一个基因子集的成员,其中uorf的修饰代表了一个重要的疾病机制。只有少数研究报道了AR基因的非编码突变,我们的病例强调了对AIS患者整个AR位点进行分子检测的重要性。在常规遗传诊断中引入综合分子检测的新方法,并结合新的分子分析工具,可以提高AIS和DSD的遗传诊断水平。
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来源期刊
CiteScore
1.00
自引率
0.00%
发文量
0
审稿时长
>12 weeks
期刊介绍: Balkan Journal of Medical Genetics is a journal in the English language for publication of articles involving all branches of medical genetics: human cytogenetics, molecular genetics, clinical genetics, immunogenetics, oncogenetics, pharmacogenetics, population genetics, genetic screening and diagnosis of monogenic and polygenic diseases, prenatal and preimplantation genetic diagnosis, genetic counselling, advances in treatment and prevention.
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