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Mutation spectrum of the bestrophin-1 gene in a large Chinese cohort with bestrophinopathy

医学 遗传学 队列 突变 基因 生物 眼科 内科学
作者
Fengjuan Gao,Yu-He Qi,Fangyuan Hu,Dandan Wang,Ping Xu,Jingli Guo,Jiankang Li,Yong-Jin Zhang,Wei Li,Fang Chen,Gezhi Xu,Wei Liu,Qing Chang,Jihong Wu
出处
期刊:British Journal of Ophthalmology [BMJ]
卷期号:104 (6): 846-851 被引量:29
标识
DOI:10.1136/bjophthalmol-2019-314679
摘要

Bestrophin-1 (BEST1) gene is associated with a wide range of ocular phenotypes, collectively termed as bestrophinopathy. The aim of the current study was to identify the mutation spectrum of BEST1 in a large cohort of Chinese patients with bestrophinopathy. Patients clinically suspected of bestrophinopathy were screened using multigene panel testing. All BEST1 variants were confirmed by Sanger sequencing, and validated in the families. A total of 92 patients (Best vitelliform macular dystrophy (BVMD)=77; autosomal recessive bestrophinopathy (ARB)=15) from 58 unrelated families of Chinese origin and their available family members (n=65) were recruited. Overall, 39 distinct disease-causing BEST1 variants were identified, including 13 novel variants, and two reported variants but novel for ARB. Of them, 14 were associated with ARB, 23 with BVMD and two (c.604C>T and c.898G>A) with both BVMD and ARB. Most mutations associated with BVMD were missense (97.78%), while ARB was associated with more complex mutations, including missense (88.46%), splicing effect (3.85%), and frameshifts (15.38%). BEST1 hotspots were c.898G>A and c.584C>T among BVMD and ARB patients, respectively. Hot regions were located in exons 8, 2 and 6 in BVMD patients, and in exons 5 and 7 in ARB patients. The overall penetrance of BEST1 in our cohort was 71.30%, no de novo mutations were identified. This is the largest study to date that provides major population-based data of the BEST1 mutation spectrum in China. Our results can serve as a well-founded reference for genetic counselling for patients with bestrophinopathy of Chinese origin.
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