TSC2基因低比例变异嵌合体致结节性硬化症1例基因学分析及产前诊断

doi:10.35541/cjd.20240480

中华皮肤科杂志 ›› 2026, e20240480.doi: 10.35541/cjd.20240480

• 研究报道 • 上一篇

TSC2基因低比例变异嵌合体致结节性硬化症1例基因学分析及产前诊断

王建波¹ 张梦瑶¹ 郑珂¹ 杨科² 宋静卉¹ 刘鸿伟¹ 李建国¹

¹河南省人民医院河南大学人民医院郑州大学人民医院皮肤科，郑州 450003；²河南省人民医院河南大学人民医院郑州大学人民医院医学遗传所，郑州 450003

收稿日期:2024-09-06 修回日期:2026-03-12 发布日期:2026-04-23
通讯作者: 李建国 E-mail:drljg006@163.com
基金资助:
河南省卫生健康委中青年学科带头人

Genetic analysis and prenatal diagnosis of a case of tuberous sclerosis complex caused by low?level mosaicism in the TSC2 gene

Wang Jianbo¹, Zhang Mengyao¹, Zheng Ke¹, Yang Ke², Song Jinghui¹, Liu Hongwei¹, Li Jianguo¹

¹Department of Dermatology, Henan Provincial People's Hospital, Henan University People's Hospital, Zhengzhou University People's Hospital, Zhengzhou 450003, China; ²Institute of Medical Genetics, Henan Provincial People's Hospital, Henan University People's Hospital, Zhengzhou University People's Hospital, Zhengzhou 450003, China

Received:2024-09-06 Revised:2026-03-12 Published:2026-04-23
Contact: Li Jianguo E-mail:drljg006@163.com
Supported by:
Henan Health Young and Middle?aged Discipline Leader Training Project

摘要/Abstract

摘要： 【摘要】目的分析1例TSC2基因发生体细胞镶嵌变异导致结节性硬化症（TSC）患者的临床特点与基因变异情况，并指导产前诊断。方法 2022年8月在河南省人民医院遗传所收集1例临床拟诊TSC患者及其父母外周血，提取DNA，先后采用全外显子组测序、全基因组高分辨率光学图谱、TSC1/TSC2基因全长测序等方法查找基因变异位点，根据高深度测序中野生型和变异型等位基因检出次数计算患者体细胞中该变异嵌合比例；同时对患者及其父母外周血DNA、患者正常皮肤组织及皮损组织DNA进行Sanger测序验证。采集患者配偶外周血及其胎儿羊水提取DNA，采用PCR扩增 + Sanger测序法对TSC2基因目标变异位点进行检测。结果患者男，26岁，背部色素减退斑26年，面部血管纤维瘤22年，趾甲甲周纤维瘤10年。其父母及其配偶既往体健，无类似症状。TSC1/TSC2基因全长测序显示，患者TSC2基因c.774+1G>A杂合变异，嵌合比例约8.86%。患者父母外周血DNA不存在此变异位点，患者正常皮肤组织及皮损组织（面部血管纤维瘤、甲周纤维瘤）DNA均存在此变异位点，Sanger测序图显示为微小突变峰。患者配偶外周血及其胎儿羊水DNA均未发现此变异位点，婴儿出生1年余，随访未发现生长发育、皮肤及神经系统任何异常表现。结论 TSC2基因发生体细胞镶嵌变异c.774+1G>A是导致该患者结节性硬化症表型的原因，促进明确致病变异位点可有效指导产前诊断、优生优育。

关键词: 结节性硬化症, TSC2基因, 镶嵌变异, 低比例变异, 产前诊断, 皮肤表现

Abstract: 【Abstract】 Objective To analyze the clinical characteristics of and gene mutation in a patient with tuberous sclerosis complex （TSC） caused by somatic mosaicism in the TSC2 gene, and to provide guidance for prenatal diagnosis. Methods In August 2022, peripheral blood samples were collected from a patient with clinically suspected TSC and his parents at the Institute of Medical Genetics, Henan Provincial People's Hospital, and DNA was extracted. Whole exome sequencing, whole genome high resolution optical mapping, and full length TSC1/TSC2 gene sequencing were sequentially performed to identify the genetic variant, and the proportion of the mosaic variant in the patient′s somatic cells was calculated based on the frequencies of the wild type and variant alleles in high depth sequencing. Sanger sequencing was performed to validate the variant in peripheral blood DNA from the patient and his parents, as well as in DNA from the patient′s normal skin tissues and lesional skin tissues. DNA was extracted from the peripheral blood and amniotic fluid of the patient′s spouse, and the target variant in the TSC2 gene was detected by PCR and Sanger sequencing. Results The 26-year-old male patient presented with hypopigmented macules on the back for 26 years, facial angiofibromas for 22 years, and periungual fibromas on the toes for 10 years. His parents and spouse were healthy with no similar symptoms. Full-length TSC1/TSC2 gene sequencing revealed a heterozygous mutation c.774+1G>A in the TSC2 gene in the patient, with a mosaic proportion of approximately 8.86%. This variant was absent in the peripheral blood DNA of the patient′s parents, but existed in DNA from the patient′s normal skin tissues and lesional skin tissues （facial angiofibromas and periungual fibromas）, with Sanger sequencing chromatograms showing a minor mutant peak. The variant was not detected in peripheral blood DNA from the patient′s spouse or in DNA from amniotic fluid. The infant had been followed up for over one year since birth, with no abnormalities in growth, development, skin, or nervous system. Conclusions The somatic mosaic mutation c.774+1G>A in the TSC2 gene was the cause of the TSC phenotype in this patient. Identification of the pathogenic variant can effectively guide prenatal diagnosis and promote healthy birth and fetal development.

Key words: Tuberous sclerosis complex, TSC2 gene, Mosaic mutation, Low proportional mutation, Prenatal diagnosis, Skin manifestations

王建波张梦瑶郑珂杨科宋静卉刘鸿伟李建国. TSC2基因低比例变异嵌合体致结节性硬化症1例基因学分析及产前诊断[J]. 中华皮肤科杂志, 2026,e20240480. doi:10.35541/cjd.20240480

Wang Jianbo, Zhang Mengyao, Zheng Ke, Yang Ke, Song Jinghui, Liu Hongwei, Li Jianguo. Genetic analysis and prenatal diagnosis of a case of tuberous sclerosis complex caused by low?level mosaicism in the TSC2 gene[J]. Chinese Journal of Dermatology,2026,e20240480. doi:10.35541/cjd.20240480

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TSC2基因低比例变异嵌合体致结节性硬化症1例基因学分析及产前诊断

Genetic analysis and prenatal diagnosis of a case of tuberous sclerosis complex caused by low?level mosaicism in the TSC2 gene

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