小眼症
发育不全
生物
外显子组
遗传学
6号乘客
遗传异质性
外显子组测序
无眼症
错义突变
基因座(遗传学)
表型
无虹膜
突变
基因
外显子
全球发育迟缓
转录因子
作者
Celia Zazo-Seco,Julie Plaisancié,Pierre Bitoun,Marta Cortón,Ana Arteche‐López,Carmen Ayuso,Adele Schneider,Dimitra Zafeiropoulou,Christian Gilissen,Olivier Roche,Felix Frémont,Patrick Calvas,Anne Slavotinek,Nicola Ragge,Nicolas Chassaing
标识
DOI:10.1038/s10038-020-0726-x
摘要
Microphthalmia, anophthalmia, and anterior segment dysgenesis are severe ocular developmental defects. There is a wide genetic heterogeneity leading to these ocular malformations. By using whole genome, exome and targeted sequencing in patients with ocular developmental anomalies, six biallelic pathogenic variants (including five novel variants) were identified in the PXDN gene in four families with microphthalmia and anterior segment dysgenesis. Only 11 different mutations (11 families) have been described in this gene to date. The phenotype of these patients is variable in severity, ranging from cataract and developmental glaucoma to complex microphthalmia. Interestingly, two unrelated patients of our series presented with an ocular phenotype including aniridia and microspherophakia. However, despite various phenotypic presentations and types of mutations, no genotype-phenotype correlation could be made. Thus, this work improves our knowledge of the recessive phenotype associated with biallelic variants in this gene and highlights the importance of screening PXDN in patients with anterior segment dysgenesis with or without microphthalmia.
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