Next-generation sequencing-based comprehensive molecular analysis of 43 Japanese patients with cone and cone-rod dystrophies.

ABCA4型 外显子组测序 生物 遗传学 色素性视网膜炎 外显子组 DNA测序 复合杂合度 生物信息学 桑格测序 疾病基因鉴定 基因 突变 古西亚德 遗传异质性 候选基因 表型 鸟苷酸环化酶2C 受体 鸟苷酸环化酶
作者
Maho Oishi,Akio Oishi,Noriko Gotoh,Ken Ogino,Koichiro Higasa,Kei Iida,Yukiko Makiyama,Shigenori Morooka,Fumihiko Matsuda,Nagahisa Yoshimura
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期刊:PubMed 卷期号:22: 150-60 被引量:15
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To investigate the efficacy of targeted exome sequencing for mutational screening of Japanese patients with cone dystrophy (CD) or cone-rod dystrophy (CRD).DNA samples from 43 Japanese patients with CD or CRD were sequenced using an exome-sequencing panel targeting all 193 known inherited eye disease genes and next-generation sequencing methodologies. Subsequently, candidate variants were screened using systematic data analyses, and their potential pathogenicity was assessed using distinct filtering approaches, which included the frequency of the variants in normal populations, in silico prediction tools, and cosegregation.Causative mutations were detected in 12 patients with CD or CRD (27.9%). In total, 14 distinct mutations were identified in the genes ABCA4, CDHR1, CRB1, CRX, GUCY2D, KCNV2, PROM1, PRPH2, and RDH5, including four novel mutations, c.3050+1G>A in ABCA4, c.386A>G in CDHR1, c.652+1_652+4del in CRB1, and c.454G>A in KCNV2. Moreover, a putative pathogenic mutation was identified in RGS9BP, a gene recognized as the source of bradyopsia.Targeted exome sequencing effectively identified causative mutations in Japanese patients with CD or CRD. The results confirmed the heterogeneity of the genes responsible for CD and CRD in Japanese populations, as well as the efficacy of targeted exome sequencing-based screening of patients with inherited retinal degeneration.

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