由CNGA3基因中的新型错义突变引起的色盲症。
Achromatopsia caused by novel missense mutations in the CNGA3 gene.
作者信息
Chen Xi-Teng, Huang Hui, Chen Yan-Hua, Dong Li-Jie, Li Xiao-Rong, Zhang Xiao-Min
机构信息
Tianjin Medical University Eye Hospital, Eye Institute & School of Optometry and Ophthalmology, Tianjin 300384, China.
BGI Health Service Co., Ltd. Airport Industrial Zone, Tianjin 300308, China.
出版信息
Int J Ophthalmol. 2015 Oct 18;8(5):910-5. doi: 10.3980/j.issn.2222-3959.2015.05.10. eCollection 2015.
AIM
To identify the genetic defects in a Chinese family with achromatopsia.
METHODS
A 2.5-year-old boy, who displayed nystagmus, photophobia, and hyperopia since early infancy, was clinically evaluated. To further confirm and localize the causative mutations in this family, targeted region capture and next-generation sequencing of candidate genes, such as CNGA3, CNGB3, GNAT2, PDE6C, and PDE6H were performed using a custom-made capture array.
RESULTS
Slit-lamp examination showed no specific findings in the anterior segments. The optic discs and maculae were normal on fundoscopy. The unaffected family members reported no ocular complaints. Clinical signs and symptoms were consistent with a clinical impression of autosomal recessive achromatopsia. The results of sequence analysis revealed two novel missense mutations in CNGA3, c.633T>A (p.D211E) and c.1006G>T (p.V336F), with an autosomal recessive mode of inheritance.
CONCLUSION
Genetic analysis of a Chinese family confirmed the clinical diagnosis of achromatopsia. Two novel mutations were identified in CNGA3, which extended the mutation spectrum of this disorder.
目的
鉴定一个患有色盲症的中国家庭的基因缺陷。
方法
对一名自婴儿早期就表现出眼球震颤、畏光和远视的2.5岁男孩进行临床评估。为了进一步确认并定位该家庭中的致病突变,使用定制捕获阵列对候选基因如CNGA3、CNGB3、GNAT2、PDE6C和PDE6H进行靶向区域捕获和二代测序。
结果
裂隙灯检查在前节未发现特异性表现。眼底检查视盘和黄斑正常。未患病的家庭成员未报告眼部不适。临床体征和症状与常染色体隐性色盲症的临床印象一致。序列分析结果显示CNGA3基因中有两个新的错义突变,c.633T>A(p.D211E)和c.1006G>T(p.V336F),呈常染色体隐性遗传模式。
结论
对一个中国家庭的基因分析证实了色盲症的临床诊断。在CNGA3基因中鉴定出两个新突变,扩展了该疾病的突变谱。
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