| Literature DB >> 30710461 |
Raquel S Silva1,2, Gavin Arno1,2, Valentina Cipriani1,2,3,4, Nikolas Pontikos1,2,4, Sabine Defoort-Dhellemmes5, Ambreen Kalhoro2, Keren J Carss6,7, F Lucy Raymond7,8, Claire Marie Dhaenens9, Hanne Jensen10, Thomas Rosenberg10, Veronica van Heyningen1,2, Anthony T Moore1,2,11, Bernard Puech5, Andrew R Webster1,2.
Abstract
The autosomal dominant progressive bifocal chorioretinal atrophy (PBCRA) disease locus has been mapped to chromosome 6q14-16.2 that overlaps the North Carolina macular dystrophy (NCMD) locus MCDR1. NCMD is a nonprogressive developmental macular dystrophy, in which variants upstream of PRDM13 have been implicated. Whole genome sequencing was performed to interrogate structural variants (SVs) and single nucleotide variants (SNVs) in eight individuals, six affected individuals from two families with PBCRA, and two individuals from an additional family with a related developmental macular dystrophy. A SNV (chr6:100,046,804T>C), located 7.8 kb upstream of the PRDM13 gene, was shared by all PBCRA-affected individuals in the disease locus. Haplotype analysis suggested that the variant arose independently in the two families. The two affected individuals from Family 3 were screened for rare variants in the PBCRA and NCMD loci. This revealed a de novo variant in the proband, 21 bp from the first SNV (chr6:100,046,783A>C). This study expands the noncoding variant spectrum upstream of PRDM13 and suggests altered spatio-temporal expression of PRDM13 as a candidate disease mechanism in the phenotypically distinct but related conditions, NCMD and PBCRA.Entities:
Keywords: NCMD; PBCRA; PRDM13; macular development; macular dystrophy; whole genome sequencing
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Year: 2019 PMID: 30710461 DOI: 10.1002/humu.23715
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878