论文信息 - Union Makes Strength: A Worldwide Collaborative Genetic and Clinical Study to Provide a Comprehensive Survey of RD3 Mutations and Delineate the Associated Phenotype - 字舞流文

Union Makes Strength: A Worldwide Collaborative Genetic and Clinical Study to Provide a Comprehensive Survey of RD3 Mutations and Delineate the Associated Phenotype

Leber congenital amaurosis (LCA) is the earliest and most severe retinal degeneration (RD), and the most common cause of incurable blindness diagnosed in children. It is occasionally the presenting symptom of multisystemic ciliopathies which diagnosis will require a specific care of patients. Nineteen LCA genes are currently identified and three of them account for both non-syndromic and syndromic forms of the disease. RD3 (LCA12) was implicated as a LCA gene based on the identification of homozygous truncating mutations in two LCA families despite the screening of large cohorts of patients. Here we provide a comprehensive survey of RD3 mutations and of their clinical expression through the screening of a cohort of 852 patients originating worldwide affected with LCA or early-onset and severe RD. We identified three RD3 mutations in seven unrelated consanguineous LCA families - i.e., a 2 bp deletion and two nonsense mutations – predicted to cause complete loss of function. Five families originating from the Southern Shores of the Mediterranean segregated a similar mutation (c.112C>T, p.R38*) suggesting that this change may have resulted from an ancient founder effect. Considering the low frequency of RD3 carriers, the recurrence risk for LCA in non-consanguineous unions is negligible for both heterozygote and homozygote RD3 individuals. The LCA12 phenotype in our patients is highly similar to those of patients with mutant photoreceptor-specific guanylate cyclase (GUCY2D/LCA1). This observation is consistent with the report of the role of RD3 in trafficking of GUCYs and gives further support to a common mechanism of photoreceptor degeneration in LCA12 and LCA1, i.e., inability to increase cytoplasmic cGMP concentration in outer segments and thus to recover the dark-state. Similar to LCA1, LCA12 patients have no extraocular symptoms despite complete inactivation of both RD3 alleles, supporting the view that extraocular investigations in LCA infants with RD3 mutations should be avoided.

A. Munnich | A. D. den Hollander | F. Cremers | A. Mégarbané | Rui Chen | S. Banfi | Xia Wang | B. Wissinger | A. Bergen | R. Gonzàlez-Duarte | S. Kohl | D. Zobor | I. Lopez | H. Ren | R. Koenekoop | F. Testa | F. Simonelli | Shi-qiang Li | Qingjiong Zhang | R. Florijn | I. Perrault | N. Delphin | J. Kaplan | J. Rozet | E. Pomares | A. Estrada-Cuzcano | R. Zekveld-Vroon | J. Andorf | N. Aboussair | C. Edelson | Marc Jean-Pierre | C. Leowski | C. Villanueva | Blanca C. Flores | E. Stone | Jeaneen Andorf

[1] M. Naash,et al. Impaired Association of Retinal Degeneration-3 with Guanylate Cyclase-1 and Guanylate Cyclase-activating Protein-1 Leads to Leber Congenital Amaurosis-1* , 2014, The Journal of Biological Chemistry.

[2] L. Molday,et al. Insights into the role of RD3 in guanylate cyclase trafficking, photoreceptor degeneration, and Leber congenital amaurosis , 2014, Front. Mol. Neurosci..

[3] Marni J. Falk,et al. NMNAT1 mutations cause Leber congenital amaurosis , 2012, Nature Genetics.

[4] Colin A. Johnson,et al. Mutations in NMNAT1 cause Leber congenital amaurosis and identify a new disease pathway for retinal degeneration , 2012, Nature Genetics.

[5] A. Munnich,et al. Mutations in NMNAT1 cause Leber congenital amaurosis with early-onset severe macular and optic atrophy , 2012, Nature Genetics.

[6] Renhua Wu,et al. Exome sequencing identifies NMNAT1 mutations as a cause of Leber congenital amaurosis , 2012, Nature Genetics.

[7] B. Lorenz,et al. Mutations in RD3 are associated with an extremely rare and severe form of early onset retinal dystrophy. , 2012, Investigative ophthalmology & visual science.

[8] V. Plagnol,et al. Recessive mutations in KCNJ13, encoding an inwardly rectifying potassium channel subunit, cause leber congenital amaurosis. , 2011, American journal of human genetics.

[9] S. Jacobson,et al. IQCB1 mutations in patients with leber congenital amaurosis. , 2011, Investigative ophthalmology & visual science.

[10] V. Sheffield,et al. Variations in NPHP5 in patients with nonsyndromic leber congenital amaurosis and Senior-Loken syndrome. , 2011, Archives of ophthalmology.

[11] L. Molday,et al. RD3, the protein associated with Leber congenital amaurosis type 12, is required for guanylate cyclase trafficking in photoreceptor cells , 2010, Proceedings of the National Academy of Sciences.

[12] F. Coppieters,et al. CEP290, a gene with many faces: mutation overview and presentation of CEP290base , 2010, Human mutation.

[13] Artur V. Cideciyan,et al. Leber congenital amaurosis due to RPE65 mutations and its treatment with gene therapy , 2010, Progress in Retinal and Eye Research.

[14] J. Kaplan,et al. Première observation maghrébine d’amaurose congénitale de Leber secondaire à une mutation du gène CEP290 , 2010 .

[15] D. Chung,et al. Leber congenital amaurosis: clinical correlations with genotypes, gene therapy trials update, and future directions. , 2009, Journal of AAPOS : the official publication of the American Association for Pediatric Ophthalmology and Strabismus.

[16] J. Lupski,et al. Mutations in SPATA7 cause Leber congenital amaurosis and juvenile retinitis pigmentosa. , 2009, American journal of human genetics.

[17] G. Acland,et al. Canine RD3 mutation establishes rod-cone dysplasia type 2 (rcd2) as ortholog of human and murine rd3 , 2009, Mammalian Genome.

[18] R. Roepman,et al. Leber congenital amaurosis: Genes, proteins and disease mechanisms , 2008, Progress in Retinal and Eye Research.

[19] J. Kaplan. Leber Congenital Amaurosis: From Darkness to Spotlight , 2008, Ophthalmic genetics.

[20] John M. Greally,et al. CG dinucleotide clustering is a species-specific property of the genome , 2007, Nucleic acids research.

[21] T. Strom,et al. Mutations in LCA5, encoding the ciliary protein lebercilin, cause Leber congenital amaurosis , 2007, Nature Genetics.

[22] A. Munnich,et al. Spectrum of NPHP6/CEP290 mutations in Leber congenital amaurosis and delineation of the associated phenotype , 2007, Human mutation.

[23] J. D. Bronson,et al. The Function of Guanylate Cyclase 1 and Guanylate Cyclase 2 in Rod and Cone Photoreceptors* , 2007, Journal of Biological Chemistry.

[24] Subhadra Jalali,et al. Premature truncation of a novel protein, RD3, exhibiting subnuclear localization is associated with retinal degeneration. , 2006, American journal of human genetics.

[25] T. Meitinger,et al. Mutations in the CEP290 (NPHP6) gene are a frequent cause of Leber congenital amaurosis. , 2006, American journal of human genetics.

[26] Steven K Fisher,et al. Morphological characterization of the retinal degeneration in three strains of mice carrying the rd-3 mutation , 2005, Visual Neuroscience.

[27] R. Reinhardt,et al. Nephrocystin-5, a ciliary IQ domain protein, is mutated in Senior-Loken syndrome and interacts with RPGR and calmodulin , 2005, Nature Genetics.

[28] A. Munnich,et al. Retinal dehydrogenase 12 (RDH12) mutations in leber congenital amaurosis. , 2004, American journal of human genetics.

[29] A. Munnich,et al. Leber congenital amaurosis: Comprehensive survey of the genetic heterogeneity, refinement of the clinical definition, and genotype–phenotype correlations as a strategy for molecular diagnosis , 2004, Human mutation.

[30] A. Ciccodicola,et al. Identification and characterization of C1orf36, a transcript highly expressed in photoreceptor cells, and mutation analysis in retinitis pigmentosa. , 2003, Biochemical and biophysical research communications.

[31] A. Munnich,et al. Evidence of autosomal dominant Leber congenital amaurosis (LCA) underlain by a CRX heterozygous null allele , 2003, Journal of medical genetics.

[32] M. Mohamed,et al. Identification of a locus (LCA9) for Leber's congenital amaurosis on chromosome 1p36 , 2003, European Journal of Human Genetics.

[33] A. Munnich,et al. Evidence of a founder effect for the RETGC1 (GUCY2D) 2943DelG mutation in Leber congenital amaurosis pedigrees of Finnish origin , 2002, Human mutation.

[34] A. Munnich,et al. Complete exon-intron structure of the RPGR-interacting protein (RPGRIP1) gene allows the identification of mutations underlying Leber congenital amaurosis , 2001, European Journal of Human Genetics.

[35] K Rohrschneider,et al. Leber congenital amaurosis and retinitis pigmentosa with Coats-like exudative vasculopathy are associated with mutations in the crumbs homologue 1 (CRB1) gene. , 2001, American journal of human genetics.

[36] P. Sieving,et al. Mutations in the gene encoding lecithin retinol acyltransferase are associated with early-onset severe retinal dystrophy , 2001, Nature Genetics.

[37] T. L. McGee,et al. Null RPGRIP1 alleles in patients with Leber congenital amaurosis. , 2001, American journal of human genetics.

[38] S. Jacobson,et al. Mutations in MERTK, the human orthologue of the RCS rat retinal dystrophy gene, cause retinitis pigmentosa , 2000, Nature Genetics.

[39] C. Cepko,et al. Mutations in a new photoreceptor-pineal gene on 17p cause Leber congenital amaurosis , 2000, Nature Genetics.

[40] Heckenlively,et al. Mutations in a new photoreceptor-pineal gene on 17p cause leber congenital amaurosis. Nat gen 2000;24:79-83 , 2000, American journal of ophthalmology.

[41] A. Munnich,et al. Different functional outcome of RetGC1 and RPE65 gene mutations in Leber congenital amaurosis. , 1999, American journal of human genetics.

[42] P. Sieving,et al. Leber congenital amaurosis caused by a homozygous mutation (R90W) in the homeodomain of the retinal transcription factor CRX: direct evidence for the involvement of CRX in the development of photoreceptor function. , 1999, Human molecular genetics.

[43] C. Freund,et al. A range of clinical phenotypes associated with mutations in CRX, a photoreceptor transcription-factor gene. , 1998, American journal of human genetics.

[44] V. Sheffield,et al. De novo mutations in the CRX homeobox gene associated with Leber congenital amaurosis , 1998, Nature Genetics.

[45] E. Zrenner,et al. Mutations in RPE65 cause Leber's congenital amaurosis , 1997, Nature Genetics.

[46] D. Paslier,et al. Retinal–specific guanylate cyclase gene mutations in Leber's congenital amaurosis , 1996, Nature Genetics.

[47] Cécile Fizames,et al. A comprehensive genetic map of the human genome based on 5,264 microsatellites , 1996, Nature.

[48] T. Roderick,et al. New mouse primary retinal degeneration (rd-3). , 1993, Genomics.

[49] M. Tso,et al. An inherited retinopathy in collies. A light and electron microscopic study. , 1980, Investigative ophthalmology & visual science.

[50] S. Vainisi,et al. Rod-cone dysplasia in the collie. , 1978, Journal of the American Veterinary Medical Association.

[51] I. Perrault,et al. [First North African observation of Leber congenital amaurosis secondary to CEP290 gene mutation]. , 2010, Journal francais d'ophtalmologie.

[52] A. Munnich,et al. Population history and infrequent mutations: how old is a rare mutation? GUCY2D as a worked example , 2008, European Journal of Human Genetics.

[53] R. Lewis,et al. Spectrum and frequency of mutations in IMPDH1 associated with autosomal dominant retinitis pigmentosa and leber congenital amaurosis. , 2006, Investigative ophthalmology & visual science.

[54] J. Heckenlively,et al. Mutations in RDH12 encoding a photoreceptor cell retinol dehydrogenase cause childhood-onset severe retinal dystrophy , 2004, Nature Genetics.

[55] J. C. Vuletin,et al. A Light and Electron Microscopic Study , 1976 .