探索新型 SRD5A2 变异对 46,XY 性发育障碍的临床影响。

Yu Mao, Jian-Mei Huang, Yu-Wei Chen-Zhang, He Lin, Yu-Huan Zhang, Ji-Yang Jiang, Xue-Mei Wu, Ling Liao, Yun-Man Tang, Ji-Yun Yang
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引用次数: 0

摘要

本研究对68名类固醇5 α还原酶2(SRD5A2)缺乏症和46,XY性发育障碍(DSD)患者进行了回顾性研究。全外显子测序发现了28个SRD5A2变体,进一步分析发现了7个新型突变体。变异主要出现在第1外显子和第4外显子,特别是在烟酰胺腺嘌呤二核苷酸磷酸(NADPH)结合区。在整个队列中,有 53 名患者在四川省人民医院(中国成都)接受了初次手术。这些患者的外生殖器评分(EGS)从 2.0 到 11.0 不等,平均值为 6.8(标准差 [s.d.]:2.5)。30 名患者同意接受激素检测。他们的平均睾酮-双氢睾酮(T/DHT)比率为 49.3(标准差:23.4)。基因检测发现,四名 EGS 评分在 6 到 9 分之间的患者患有该综合征;他们的 T/DHT 比率低于诊断阈值。此外,利用人类 SRD5A2 的晶体结构进行的评估深入揭示了这些新型变异体的潜在致病机制。这些机制包括干扰 NADPH 结合(c.356G>C、c.365A>G、c.492C>G 和 c.662T>G)和破坏蛋白质结构的稳定性(c.727C>T)。经核实,c.446-1G>T 和 c.380delG 变异导致转录本发生了巨大变化。发现了 7 个新变异,并扩充了 SRD5A2 基因的变异数据库。这些发现有助于SRD5A2缺乏症患者的诊断和治疗方法的进步。
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Exploring the clinical implications of novel SRD5A2 variants in 46,XY disorders of sex development.

This study was conducted retrospectively on a cohort of 68 patients with steroid 5 α-reductase 2 (SRD5A2) deficiency and 46,XY disorders of sex development (DSD). Whole-exon sequencing revealed 28 variants of SRD5A2, and further analysis identified seven novel mutants. The preponderance of variants was observed in exon 1 and exon 4, specifically within the nicotinamide adenine dinucleotide phosphate (NADPH)-binding region. Among the entire cohort, 53 patients underwent initial surgery at Sichuan Provincial People's Hospital (Chengdu, China). The external genitalia scores (EGS) of these participants varied from 2.0 to 11.0, with a mean of 6.8 (standard deviation [s.d.]: 2.5). Thirty patients consented to hormone testing. Their average testosterone-to-dihydrotestosterone (T/DHT) ratio was 49.3 (s.d.: 23.4). Genetic testing identified four patients with EGS scores between 6 and 9 as having this syndrome; and their T/DHT ratios were below the diagnostic threshold. Furthermore, assessments conducted using the crystal structure of human SRD5A2 have provided insights into the potential pathogenic mechanisms of these novel variants. These mechanisms include interference with NADPH binding (c.356G>C, c.365A>G, c.492C>G, and c.662T>G) and destabilization of the protein structure (c.727C>T). The c.446-1G>T and c.380delG variants were verified to result in large alterations in the transcripts. Seven novel variations were identified, and the variant database for the SRD5A2 gene was expanded. These findings contribute to the progress of diagnostic and therapeutic approaches for individuals with SRD5A2 deficiency.

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