Whole genome sequencing in patients with retinitis pigmentosa reveals pathogenic DNA structural changes and NEK2 as a new disease gene

We performed whole genome sequencing in 16 unrelated patients with autosomal recessive retinitis pigmentosa (ARRP), a disease characterized by progressive retinal degeneration and caused by mutations in over 50 genes, in search of pathogenic DNA variants. Eight patients were from North America, wher...

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Published in:Proceedings of the National Academy of Sciences - PNAS Vol. 110; no. 40; pp. 16139 - 16144
Main Authors: Nishiguchi, Koji M., Tearle, Richard G., Liu, Yangfan P., Oh, Edwin C., Miyake, Noriko, Benaglio, Paola, Harper, Shyana, Koskiniemi-Kuendig, Hanna, Venturini, Giulia, Sharon, Dror, Koenekoop, Robert K., Nakamura, Makoto, Kondo, Mineo, Ueno, Shinji, Yasuma, Tetsuhiro R., Beckmann, Jacques S., Ikegawa, Shiro, Matsumoto, Naomichi, Terasaki, Hiroko, Berson, Eliot L., Katsanis, Nicholas, Rivolta, Carlo
Format: Journal Article
Language:English
Published: United States National Academy of Sciences 01-10-2013
NATIONAL ACADEMY OF SCIENCES
National Acad Sciences
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Summary:We performed whole genome sequencing in 16 unrelated patients with autosomal recessive retinitis pigmentosa (ARRP), a disease characterized by progressive retinal degeneration and caused by mutations in over 50 genes, in search of pathogenic DNA variants. Eight patients were from North America, whereas eight were Japanese, a population for which ARRP seems to have different genetic drivers. Using a specific workflow, we assessed both the coding and noncoding regions of the human genome, including the evaluation of highly polymorphic SNPs, structural and copy number variations, as well as 69 control genomes sequenced by the same procedures. We detected homozygous or compound heterozygous mutations in 7 genes associated with ARRP (USH2A , RDH12 , CNGB1 , EYS , PDE6B , DFNB31 , and CERKL) in eight patients, three Japanese and five Americans. Fourteen of the 16 mutant alleles identified were previously unknown. Among these, there was a 2.3-kb deletion in USH2A and an inverted duplication of ∼446 kb in EYS , which would have likely escaped conventional screening techniques or exome sequencing. Moreover, in another Japanese patient, we identified a homozygous frameshift (p.L206fs), absent in more than 2,500 chromosomes from ethnically matched controls, in the ciliary gene NEK2 , encoding a serine/threonine-protein kinase. Inactivation of this gene in zebrafish induced retinal photoreceptor defects that were rescued by human NEK2 mRNA. In addition to identifying a previously undescribed ARRP gene, our study highlights the importance of rare structural DNA variations in Mendelian diseases and advocates the need for screening approaches that transcend the analysis of the coding sequences of the human genome.
Bibliography:http://dx.doi.org/10.1073/pnas.1308243110
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Author contributions: K.M.N. and C.R. designed research; K.M.N., Y.P.L., E.C.O., N. Miyake, P.B., H.K.-K., and G.V. performed research; S.H., D.S., R.K.K., M.N., M.K., S.U., T.R.Y., S.I., N. Matsumoto, H.T., and E.L.B. contributed new reagents/analytic tools; K.M.N., R.G.T., Y.P.L., E.C.O., N. Miyake, P.B., H.K.-K., G.V., J.S.B., S.I., N. Matsumoto, N.K., and C.R. analyzed data; and K.M.N., E.C.O., J.S.B., E.L.B., N.K., and C.R. wrote the paper.
Edited by Jeremy Nathans, Johns Hopkins University, Baltimore, MD, and approved August 15, 2013 (received for review May 1, 2013)
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1308243110