Description and molecular analysis of SRY and AR genes in a patient with 46,XY pure gonadal dysgenesis (Swyer syndrome)

Annales de Génétique Pub Date : 2004-04-01 DOI:10.1016/j.anngen.2003.08.022

Dimitrios Iliopoulos, Nikolaos Volakakis, Alexandra Tsiga, Israel Rousso, Nikolaos Voyiatzis

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引用次数: 12

Abstract

46,XY pure gonadal dysgenesis, first described in 1955 by Swyer, results from testicular tissue loss during the first 8 weeks of fetal life, a critical period for male differentiation. We describe a case of an 18 years old patient presented to us with a chief complain of primary amenorrhea. Chromosomal analysis revealed a 46,XY karyotype. A molecular investigation was undertaken in an attempt to determine mutations in SRY and AR genes through DNA sequencing. Mutations were shown to be absent. The molecular basis of Swyer syndrome is still unknown, although the presence of mutations in testicular organizing genes downstream of SRY is still to rule out. The patient, who is considered as female, was placed on estrogen replacement therapy, while bilateral prophylactic laparoscopic gonadectomy was programmed due to the high prevalence of gonadal tumors in this syndrome. No signs of malignance were detected in the gonadal tissue, which predicts that an intact SRY gene is usually, but not always, not related to the formation of malignancies like dysgeminomas or gonadoblastomas.

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一例46,xy纯性腺发育不良(Swyer综合征)患者的SRY和AR基因描述及分子分析

46、XY纯性腺发育不良，由Swyer于1955年首次描述，是由于胎儿生命的前8周睾丸组织丢失造成的，这是男性分化的关键时期。我们描述的情况下，一个18岁的病人提出了我们的主要抱怨原发性闭经。染色体分析显示为46,xy核型。我们进行了分子研究，试图通过DNA测序确定SRY和AR基因的突变。突变被证明是缺失的。Swyer综合征的分子基础尚不清楚，尽管仍不能排除SRY下游睾丸组织基因突变的存在。该患者被认为是女性，接受雌激素替代治疗，同时由于该综合征中性腺肿瘤的高患病率，计划进行双侧预防性腹腔镜性腺切除术。在性腺组织中未发现恶性肿瘤的迹象，这预示着一个完整的SRY基因通常(但并非总是)与恶性肿瘤的形成，如双胞异构瘤或性腺母细胞瘤无关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Annales de Génétique

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