Clinical and genetic characteristics of 251 consecutive patients with macular and cone/cone-rod dystrophy

Birtel, Johannes; Eisenberger, Tobias; Gliem, Martin; Müller, Philipp L.; Herrmann, Philipp; Betz, Christian; Zahnleiter, Diana; Neuhaus, Christine; Lenzner, Steffen; Holz, Frank G.; Mangold, Elisabeth; Bolz, Hanno J.; Issa, Peter Charbel

doi:10.1038/s41598-018-22096-0

Cited by 149 publications

(140 citation statements)

References 68 publications

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“…There are currently 261 genes listed with established links to RDs (http://www.sph.uth.tmc.edu/RetNet/). Several studies have shown a rather high diagnostic yield (50%‐79%) of multigene panels in patients with RD . However, those cohorts were not selected on the basis of a particular mode of inheritance.…”

Section: Introductionmentioning

confidence: 99%

Mutations in known disease genes account for the majority of autosomal recessive retinal dystrophies

Patel

Alkuraya²,

Alzahrani

et al. 2018

Clinical Genetics

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Retinal dystrophies (RDs) are hereditary blinding eye conditions that are highly variable in their clinical presentation. The remarkable genetic heterogeneity that characterizes RD was a major challenge in establishing the molecular diagnosis in these patients until the recent advent of next-generation sequencing. It remains unclear, however, what percentage of autosomal recessive RD remain undiagnosed when all established RD genes are sequenced. We enrolled 75 families in which RD segregates in an apparently autosomal recessive manner. We show that the yield of a multigene panel that contains known RD genes is 67.5%. The higher yield (82.3%) when whole exome sequencing was implemented instead was often due to hits in genes that were not included in the original design of the panel. We also show the value of homozygosity mapping even during the era of exome sequencing in uncovering cryptic mutations. In total, we describe 45 unique likely deleterious variants (of which 18 are novel including one deep intronic and one genomic deletion mutation). Our study suggests that the genetic heterogeneity of autosomal recessive RD is approaching saturation and that any new RD genes will probably account for only a minor role in the mutation burden.

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Section: Introductionmentioning

confidence: 99%

Mutations in known disease genes account for the majority of autosomal recessive retinal dystrophies

Patel

Alkuraya²,

Alzahrani

et al. 2018

Clinical Genetics

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“…In literatures, different autosomal recessive phenotypes have been associated with the CDHR1 gene mutations, ranging from RP to CRD although the relationship between phenotypes and gene mutations are variable . The proband in our study, with a loss of more than one‐thirds of CDHR1 by a homozygous and nonsense variant p.Y547*, has been noticed the simultaneous onset of dark adaptation difficulties, trouble with color vision, and light sensitivity at age of 24; ERG in different waves showed markedly reduced rod‐and‐cone responses; FP/FPP showed macular dysdrophy (MD).…”

Section: Discussionmentioning

confidence: 51%

“…Clinically, this patient presented MD/CRD. Thus, combined with our study, patients with CDHR1 truncated protein by nonsense, splicing variants or deletions with frameshift, other than missense variants, might cause more severely phenotypes, such as MD/CRD, and/or earlier disease onset …”

Section: Discussionmentioning

confidence: 53%

“…The pathogenic CDHR1 mutation was first identified in 2010, and only a few mutations have been reported since then . Very recently, six CDHR1 mutations were also identified in Germany for macular and cone/cone‐rod dystrophies or retinal dystrophy . These small amounts of mutations suggest that the mutations in the CDHR1 gene are a rare case of arCRD (autosomal recessive cone‐rod dystrophy) in Western countries .…”

Section: Discussionmentioning

confidence: 99%

“…Here, we applied targeted next‐generation sequencing (TGS) technology, the most available ‎and promising method available, to identify a novel, homologous mutation of CDHR1 gene in a Chinese family with autosomal recessive retinal dystrophy, extending the gene's mutation spectrum.…”

Section: Introductionmentioning

confidence: 99%

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A novel, homozygous nonsense variant of the CDHR1 gene in a Chinese family causes autosomal recessive retinal dystrophy by NGS‐based genetic diagnosis

Cheng

et al. 2018

J Cellular Molecular Medi

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Retinal dystrophy is an inherited, heterogeneous, chronic and progressive disorder of visual functions. The mutations of patients with autosomal recessive retinal retinopathy cone‐and‐rod dysfunction and macular dystrophy have not been well described in the Chinese population. In this study, a three‐generation Chinese retinal dystrophy family was recruited. Ophthalmic examinations were performed. Targeted next generation sequencing (TGS) was used to identify causative genes, and Sanger sequencing was conducted to verify candidate mutations and co‐segregation. Reverse transcription (RT)‐PCR was applied to investigate the spatial and temporal expression patterns of cdhr1 gene in mouse. A novel, homozygous, deleterious and nonsense variant (c.T1641A; p.Y547*) in the CDHR1 gene was identified in the family with autosomal recessive retinal dystrophy, which was co‐segregated with the clinical phenotypes in this family. RT‐PCR analysis revealed that cdhr1 is ubiquitously expressed in eye, particularly very high expression in retina; high expression in lens, sclera, and cornea; and high expression in brain. In conclusion, our study is the first to indicate that the novel homozygous variant c.T1641A (p.Y547*) in the CHDR1 gene might be the disease‐causing mutation for retinal dystrophy in our patient, extending its mutation spectrums. These findings further the understanding of the molecular pathogenesis of this disease and provide new insights for diagnosis as well as new implications for genetic counselling.

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Clinical and Molecular Characterization ofPROM1-Related Retinal Degeneration

et al. 2019

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Key Points Question What are the clinical and molecular characteristics of PROM1- related retinal degeneration? Findings In this case series of 19 patients with PROM1 -related retinal degeneration, recessive variants were associated with early-onset, severe panretinal degeneration, whereas the dominant disease was associated with the c.1117C>T variant and a late-onset, milder phenotype that predominantly involves the macula. In addition, the dominant variant was preferentially associated with cone photoreceptors. Meaning A better understanding of the clinical and molecular characteristics of PROM1- related retinal degeneration may aid development of future treatments, including gene therapy and optogenetics.

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Clinical and genetic characteristics of 251 consecutive patients with macular and cone/cone-rod dystrophy

Cited by 149 publications

References 68 publications

Mutations in known disease genes account for the majority of autosomal recessive retinal dystrophies

Mutations in known disease genes account for the majority of autosomal recessive retinal dystrophies

A novel, homozygous nonsense variant of the CDHR1 gene in a Chinese family causes autosomal recessive retinal dystrophy by NGS‐based genetic diagnosis

Clinical and Molecular Characterization ofPROM1-Related Retinal Degeneration

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