一例智力障碍和语言发育迟缓患儿的STAG1基因变异分析

doi:10.16288/j.yczz.25-130

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Hereditas(Beijing) ›› 2026, Vol. 48 ›› Issue (2): 227-235.doi: 10.16288/j.yczz.25-130

• Genetic Resource • Previous Articles

Analysis of STAG1 gene variants identified in a patient with intellectual disability and speech delay

Cuicui Jiang¹(), Ke Wu²()

1. Obstetrics Department, Quzhou Maternity and Child Health Care Hospital of Zhejiang Province, Quzhou 32400, China
2. Laboratory of Prenatal Diganosis Center, Quzhou Maternity and Child Health Care Hospital of Zhejiang Province, Quzhou 32400, China

Received:2025-05-19 Revised:2025-07-08 Online:2025-07-30 Published:2025-07-30
Contact: Ke Wu E-mail:18268961535@163.com;13277989175@163.com

Abstract

Abstract:

Autosomal dominant intellectual developmental disorder (type 47) (OMIM #617635) is associated with heterozygous variants in the STAG1 gene (OMIM*604358). The main clinical manifestations include intellectual disability, delayed language development, abnormal facial features, epilepsy, etc. In this study, we performed the whole-exome sequencing (WES) on a 3-year-old child diagnosed with psychomotor developmental delay, and verified candidate gene variants by Sanger sequencing. We constructed a mutant plasmid expression vector and subsequently transfected it into HEK293T cells to preliminarily investigate the pathogenic mechanism of the identified variant. Additionally, we conducted a comprehensive review of previously published literature to systematically summarize the associated clinical phenotypes. WES revealed that the patient harbored the c.500dup (p.Gly168TrpfsTer13) of the STAG1 gene, and it was a de novo variant. Based on the guidelines from the American College of Medical Genetics and Genomics (ACMG), the variant was classified as a pathogenic variant (PVS1+PM2_Supporting+PS2_Supporting). In vitro cellular function studies have demonstrated that this variant resulted in a substantial decrease in the expression of mutant mRNA, thereby impairing the production of functional STAG1 protein. Clinical phenotypes associated with STAG1 gene variants display considerable variability. This study suggests that the pathogenic mechanism of STAG1 gene variants may be linked to haploinsufficiency of the gene.

Key words: STAG1 gene, intellectual disability, delayed speech, whole-exome sequencing, haploinsufficiency

Cuicui Jiang, Ke Wu. Analysis of STAG1 gene variants identified in a patient with intellectual disability and speech delay[J]. Hereditas(Beijing), 2026, 48(2): 227-235.

Figures/Tables 8

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Table 1

Summary of the clinical phenotypes of children with STAG1 gene variants"

STAG1基因变异信息(NM_005862.2)	产前表型	产后表型	参考文献
c.641A>G (p.Gln214Arg)	无明显异常	9岁，男性，智力障碍，语言发育迟缓，轻度听力丧失，面容异常，头围偏小(-1SD)	[1]
c.1433A>C (p.His478Pro)	无明显异常	脊柱侧弯；脑MRI提示脑萎缩
c.646A>G (p.Arg216Gly)	无明显异常	面容异常,头围偏小(-1.5 SD)
c.1118G>A (p.Arg373Gln)	无明显异常	睡眠障碍
c.1460_1464dup (p.Trp489Valfs*10)	无明显异常	头围正常
c.659A>G (p.His220Arg)	无明显异常	睡眠障碍
c.997A>C (p.Lys333Gln)	无明显异常	隐睾症
c.2936A>G (p.Lys979Arg)	无明显异常	头围正常
c.1052T>G (p.Leu351Trp)	无明显异常	面容无明显异常
c.1736 (p.Ser580Valfs*21)	无明显异常	头围正常
c.2009_2012del (p.N670Ifs*25)	无明显异常	11岁，女性，智力障碍，语言发育迟缓，自闭症，面容异常，斜视，并趾，性早熟，皮肤异常	[12]
c.1129C>T (p.Arg377Cys)	NA	并趾	[12]
c.2769_2770del (p.Ile924Serfs*8)	无明显异常	5岁，女性，发育迟缓，智力障碍，语言发育迟缓，反复呼吸道感染，特发性关节炎，面容异常，小头畸形，小颌畸形，胸骨凹陷，并指，第五小指弯曲	[13]
c.901C>T (p.Arg301Cys)	宫内发育迟缓	3岁，男性，全面发育迟缓(智力障碍，语言发育迟缓)，婴儿期喂养困难，身材矮小，面容异常，小头畸形，双侧小耳畸形，下颌骨发育不良，隐睾症，听力丧失	[14]
c.1279G>A (p.Val427Ile)	无明显异常	9岁，同卵双胞胎I，男性，33周早产，智力障碍，语言发育迟缓，面容异常，双侧扁平足，肥胖	[15]
c.1279G>A (p.Val427Ile)	无明显异常	肥胖	[15]
c.1183C>T, (p.Arg395*)	无明显异常	3岁，女性，发育迟缓，语言发育迟缓，面容异常，平头畸形，小颌畸形，双侧马蹄足，视力障碍	[16]
c.17T>G (p.Leu6*)	NA	发育迟缓，身材矮小，智力障碍，面容异常，多毛症，无年龄和性别信息	[17]

Table 1

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Analysis of STAG1 gene variants identified in a patient with intellectual disability and speech delay

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