Atonal homolog 7 (ATOH7) loss-of-function mutations in predominant bilateral optic nerve hypoplasia

Atac, David; Koller, Samuel; Hanson, James V M; Feil, Silke; Tiwari, Anjali; Bahr, Angela; Baehr, Luzy; Magyar, I; Kottke, Raimund; Gerth‐Kahlert, Christina; Berger, Wolfgang

doi:10.1093/hmg/ddz268

Cited by 12 publications

(26 citation statements)

References 80 publications

(82 reference statements)

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“…Human nonsyndromic congenital retinal nonattachment (NCRNA) disease is characterized by optic nerve aplasia, with profound secondary retinovascular and other ocular defects ( 26 , 27 ). The clinical phenotype overlaps autosomal recessive persistent hyperplastic primary vitreous (arPHPV) and vitreoretinal dystrophy, which are caused by point mutations in the ATOH7 coding sequence ( 18 , 26 , 28 , 29 ), and findings in Atoh7 mutant mice ( 16 , 17 , 30 ). NCRNA is caused by a 6.5-kb deletion, extending from 19.2 to 25.7 kb upstream of the TSS.…”

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confidence: 99%

TheAtoh7remote enhancer provides transcriptional robustness during retinal ganglion cell development

Miesfeld

Ghiasvand

Marsh-Armstrong

et al. 2020

Proc. Natl. Acad. Sci. U.S.A.

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The retinal ganglion cell (RGC) competence factor ATOH7 is dynamically expressed during retinal histogenesis. ATOH7 transcription is controlled by a promoter-adjacent primary enhancer and a remote shadow enhancer (SE). Deletion of the ATOH7 human SE causes nonsyndromic congenital retinal nonattachment (NCRNA) disease, characterized by optic nerve aplasia and total blindness. We used genome editing to model NCRNA in mice. Deletion of the murine SE reduces Atoh7 messenger RNA (mRNA) fivefold but does not recapitulate optic nerve loss; however, SEdel/knockout (KO) trans heterozygotes have thin optic nerves. By analyzing Atoh7 mRNA and protein levels, RGC development and survival, and chromatin landscape effects, we show that the SE ensures robust Atoh7 transcriptional output. Combining SE deletion and KO and wild-type alleles in a genotypic series, we determined the amount of Atoh7 needed to produce a normal complement of adult RGCs, and the secondary consequences of graded reductions in Atoh7 dosage. Together, these data reveal the workings of an evolutionary fail-safe, a duplicate enhancer mechanism that is hard-wired in the machinery of vertebrate retinal ganglion cell genesis.

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confidence: 99%

TheAtoh7remote enhancer provides transcriptional robustness during retinal ganglion cell development

Miesfeld

Ghiasvand

Marsh-Armstrong

et al. 2020

Proc. Natl. Acad. Sci. U.S.A.

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“…3,5,6 Likewise, an increasing number of studies highlight ATOH7 as an emerging candidate for eye diseases in humans. Variations in the ATOH7 locus have been associated with optic nerve hypoplasia (ONH) and aplasia (ONA), [8][9][10][11] further pointing towards the crucial role of atoh7 in RGC genesis and optic nerve development. Remarkably, a number of studies have also emerged, which highlight ATOH7 variants as associated with multiple eye disease traits.…”

Section: Introductionmentioning

confidence: 99%

Transcriptome analysis of the zebrafishatoh7−/−Mutant,lakritz, highlights Atoh7‐dependent genetic networks with potential implications for human eye diseases

et al. 2020

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Expression of the bHLH transcription protein Atoh7 is a crucial factor conferring competence to retinal progenitor cells for the development of retinal ganglion cells. Several studies have emerged establishing ATOH7 as a retinal disease gene. Remarkably, such studies uncovered ATOH7 variants associated with global eye defects including optic nerve hypoplasia, microphthalmia, retinal vascular disorders, and glaucoma. The complex genetic networks and cellular decisions arising downstream of atoh7 expression, and how their dysregulation cause development of such disease traits remains unknown. To begin to understand such Atoh7‐dependent events in vivo, we performed transcriptome analysis of wild‐type and atoh7 mutant ( lakritz ) zebrafish embryos at the onset of retinal ganglion cell differentiation. We investigated in silico interplays of atoh7 and other disease‐related genes and pathways. By network reconstruction analysis of differentially expressed genes, we identified gene clusters enriched in retinal development, cell cycle, chromatin remodeling, stress response, and Wnt pathways. By weighted gene coexpression network, we identified coexpression modules affected by the mutation and enriched in retina development genes tightly connected to atoh7 . We established the groundwork whereby Atoh7‐linked cellular and molecular processes can be investigated in the dynamic multi‐tissue environment of the developing normal and diseased vertebrate eye.

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“…In tetrapods, barhl2 (previously named MBH1 and XBH1) is expressed in both amacrine cells and RGCs of the developing and mature retina 12,13 . Studies have also reported that Barhl2 is both sufficient and essential for determining the subtype specific identity of amacrine cells as well as to promote the maturation and survival of RGCs downstream of Atoh7 (also known as Ath5) -a bHLH transcription factor required for the specification of RGCs in vertebrates [12][13][14][15][16][17][18] .…”

Section: Introductionmentioning

confidence: 99%

Expression of a Barhl1a reporter in subsets of retinal ganglion cells and commissural neurons of the developing zebrafish brain

Albadri

Armant

Aljand-Geschwill

et al. 2020

Preprint

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Promoting the regeneration or survival of retinal ganglion cells (RGCs) is one focus of regenerative medicine. Homeobox Barhl transcription factors might be instrumental in these processes. In mammals, only barhl2 is expressed in the retina and is required for both subtype identity acquisition of amacrine cells and for the survival of RGCs downstream of Atoh7, a transcription factor necessary for RGC genesis. The underlying mechanisms of this dual role of Barhl2 in mammals have remained elusive. Whole genome duplication in the teleost lineage generated the barhl1a and barhl2 paralogues. In the Zebrafish retina, Barhl2 functions as determinant of subsets of amacrine cells lineally related to RGCs independently of Atoh7. In contrast, barhl1a expression depends on Atoh7 but its expression dynamics and function have not been studied. Here we describe for the first time a Barhl1a:GFP reporter line in vivo showing that Barhl1a turns on exclusively in subsets of RGCs and their post-mitotic precursors. We also show transient expression of Barhl1a:GFP in diencephalic neurons extending their axonal projections as part of the post-optic commissure, at the time of optic chiasm formation. This work sets the ground for future studies on RGC subtype identity, axonal projections and genetic specification of Barhl1a-positive RGCs and commissural neurons.

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Atonal homolog 7 (ATOH7) loss-of-function mutations in predominant bilateral optic nerve hypoplasia

Cited by 12 publications

References 80 publications

TheAtoh7remote enhancer provides transcriptional robustness during retinal ganglion cell development

TheAtoh7remote enhancer provides transcriptional robustness during retinal ganglion cell development

Transcriptome analysis of the zebrafishatoh7−/−Mutant,lakritz, highlights Atoh7‐dependent genetic networks with potential implications for human eye diseases

Expression of a Barhl1a reporter in subsets of retinal ganglion cells and commissural neurons of the developing zebrafish brain

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