Trio-based exome sequencing arrests de novo mutations in early-onset high myopia

Author:

Jin Zi-BingORCID,Wu Jinyu,Huang Xiu-Feng,Feng Chun-Yun,Cai Xue-Bi,Mao Jian-Yang,Xiang Lue,Wu Kun-Chao,Xiao Xueshan,Kloss Bethany A.,Li Zhongshan,Liu Zhenwei,Huang Shenghai,Shen Meixiao,Cheng Fei-Fei,Cheng Xue-Wen,Zheng Zhi-Li,Chen Xuejiao,Zhuang Wenjuan,Zhang Qingjiong,Young Terri L.,Xie Ting,Lu Fan,Qu Jia

Abstract

The etiology of the highly myopic condition has been unclear for decades. We investigated the genetic contributions to early-onset high myopia (EOHM), which is defined as having a refraction of less than or equal to −6 diopters before the age of 6, when children are less likely to be exposed to high educational pressures. Trios (two nonmyopic parents and one child) were examined to uncover pathogenic mutations using whole-exome sequencing. We identified parent-transmitted biallelic mutations or de novo mutations in as-yet-unknown or reported genes in 16 probands. Interestingly, an increased rate of de novo mutations was identified in the EOHM patients. Among the newly identified candidate genes, a BSG mutation was identified in one EOHM proband. Expanded screening of 1,040 patients found an additional four mutations in the same gene. Then, we generated Bsg mutant mice to further elucidate the functional impact of this gene and observed typical myopic phenotypes, including an elongated axial length. Using a trio-based exonic screening study in EOHM, we deciphered a prominent role for de novo mutations in EOHM patients without myopic parents. The discovery of a disease gene, BSG, provides insights into myopic development and its etiology, which expands our current understanding of high myopia and might be useful for future treatment and prevention.

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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