Objective: To explore the clinical phenotypes and pathogenic gene variation characteristics of three Chinese Han ethnic families affected by Nance-Horan syndrome, a rare X-linked genetic disorder. Methods: A pedigree investigation study was conducted at the First Affiliated Hospital of Zhengzhou University, collecting clinical data from three Chinese Han families with Nance-Horan syndrome between February 2009 and September 2018. Detailed family histories, comprehensive ophthalmological and systemic examinations were documented. Pedigree charts were created, and genetic inheritance patterns were analyzed to preliminarily diagnose the probands and other affected individuals. Genomic DNA was extracted from peripheral blood samples of family members, and next-generation sequencing was used to screen for target gene variations, which were confirmed by Sanger sequencing. Pathogenicity of the genetic variants and their impact on three-dimensional protein structure were analyzed using MutationTaster and computer-aided protein modeling. Results: In Family 1, there are 5 patients, including 4 females (aged 42, 37, 9 and 7) and 1 males (aged 12). In Family 2, there are 5 patients, including 3 females (aged 54, 32 and 16) and 2 males (aged 26 and 9). In Family 3, there are 8 patients, including 5 females (aged 69, 42, 37, 35 and 14) and 3 males (aged 10, 7 and 4). All probands in the three families exhibited nuclear cataracts with typical congenital hereditary cataract features, but no noticeable abnormalities in facial appearance or teeth. Next-generation sequencing identified new variation sites in the NHS gene, specifically c.2519_2520del, exon3del, and c.3847C>T. These variations included nonsense mutation p.(Ser840*), exon deletion p.(?), and nonsense mutation p.(Gln1283*). Combined clinical and genetic sequencing results confirmed X-linked Nance-Horan syndrome in all three families. Bioinformatics analysis indicated these variation sites were pathogenic and resulted in abnormal three-dimensional protein structures, likely being the main cause of Nance-Horan syndrome. Conclusion: The majority of patients from the three Nance-Horan syndrome families studied were affected by congenital hereditary cataracts characterized by nuclear opacities.The NHS gene variations c.2519_2520del, exon3del, and c.3847C>T are newly identified pathogenic sites in Nance-Horan syndrome, reported for the first time across three different families.
目的: 探讨3个X连锁先天性遗传病Nance-Horan综合征家系的临床表型和致病基因变异特点。 方法: 回顾性病例系列研究。收集2009年2月至2018年9月于郑州大学第一附属医院就诊的3个中国汉族Nance-Horan综合征家系的临床资料。对相关人群进行病史采集,记录家族史,并进行眼科及全身检查。根据病史绘制系谱图并分析遗传方式,初步明确先证者及家系其他患者的诊断。采集3个家系成员外周血,提取基因组DNA,运用二代测序筛查、Sanger测序验证目标基因变异位点。结合基因变异的结果,通过序列变异解读指南、MutationTaster和计算机辅助蛋白建模方式探究基因变异的致病性分析和三维蛋白结构变化。 结果: 家系1中5例患者,其中女性4例(年龄分别为42、37、9和7岁)和男性1例(12岁)。家系2中5例患者,其中女性3例(年龄分别为54、32和16岁)和男性2例(年龄分别为26和9岁)。家系3中有8例患者,其中女性5例(年龄分别为69、42、37、35和14岁)和男性3例(年龄分别为10、7和4岁)。3个家系中先证者均表现出晶状体核性混浊,并伴有典型的先天性遗传性白内障的临床特征,面部外形和牙齿未见明显异常。二代测序后发现3个家系NHS基因均有新的变异位点,分别为c.2519_2520del、exon3del、c.3847C>T,其中家系1为无义变异p.(Ser840*)、家系2为外显子缺失变异p.(?)、家系3为无义变异p.(Gln1283*),结合临床和基因测序结果证实3个家系为X连锁遗传病Nance-Horan综合征。通过生物信息学工具分析判断变异位点具有致病性,引发三维蛋白结构异常,这可能是导致Nance-Horan综合征的主要原因。 结论: 3个Nance-Horan综合征家系大部分患者患有以核性混浊为特征的先天性遗传性白内障,其致病NHS基因c.2519_2520del、exon3del、c.3847C>T变异为Nance-Horan综合征新的致病性变异位点。.