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Robust Genetic Analysis of the X-Linked Anophthalmic ( Ie ) Mouse

Anophthalmia (missing eye) describes a failure of early embryonic ocular development. Mutations in a relatively small set of genes account for 75% of bilateral anophthalmia cases, yet 25% of families currently are left without a molecular diagnosis. Here, we report our experimental work that aimed t...

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Bibliographic Details
Published in:Genes 2022-10, Vol.13 (10), p.1797
Main Authors: Hernandez-Moran, Brianda A, Papanastasiou, Andrew S, Parry, David, Meynert, Alison, Gautier, Philippe, Grimes, Graeme, Adams, Ian R, Trejo-Reveles, Violeta, Bengani, Hemant, Keighren, Margaret, Jackson, Ian J, Adams, David J, FitzPatrick, David R, Rainger, Joe
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Language:English
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Summary:Anophthalmia (missing eye) describes a failure of early embryonic ocular development. Mutations in a relatively small set of genes account for 75% of bilateral anophthalmia cases, yet 25% of families currently are left without a molecular diagnosis. Here, we report our experimental work that aimed to uncover the developmental and genetic basis of the anophthalmia characterising the X-linked (eye-ear reduction) X-ray-induced allele in mouse that was first identified in 1947. Histological analysis of the embryonic phenotype showed failure of normal eye development after the optic vesicle stage with particularly severe malformation of the ventral retina. Linkage analysis mapped this mutation to a ~6 Mb region on the X chromosome. Short- and long-read whole-genome sequencing (WGS) of affected and unaffected male littermates confirmed the linkage but identified no plausible causative variants or structural rearrangements. These analyses did reduce the critical candidate interval and revealed evidence of multiple variants within the ancestral DNA, although none were found that altered coding sequences or that were unique to . To investigate early embryonic events at a genetic level, we then generated mouse ES cells derived from male embryos and wild type littermates. RNA-seq and accessible chromatin sequencing (ATAC-seq) data generated from cultured optic vesicle organoids did not reveal any large differences in gene expression or accessibility of putative cis-regulatory elements between and wild type. However, an unbiased TF-footprinting analysis of accessible chromatin regions did provide evidence of a genome-wide reduction in binding of transcription factors associated with ventral eye development in , and evidence of an increase in binding of the Zic-family of transcription factors, including Zic3, which is located within the -refined critical interval. We conclude that the refined critical region at chrX: 56,145,000-58,385,000 contains multiple genetic variants that may be linked to altered regulation but does not contain a convincing causative mutation. Changes in the binding of key transcription factors to chromatin causing altered gene expression during development, possibly through a subtle mis-regulation of Zic3, presents a plausible cause for the anophthalmia phenotype observed in , but further work is required to determine the precise causative allele and its genetic mechanism.
ISSN:2073-4425
2073-4425
DOI:10.3390/genes13101797