Mutation Altering the miR-184 Seed Region Causes Familial Keratoconus with Cataract

Hughes, Anne E.; Bradley, Declan; Campbell, Malcolm M.; Lechner, Judith; Dash, Durga Prasad; Simpson, David; Willoughby, Colin E.

doi:10.1016/j.ajhg.2011.09.014

Cited by 239 publications

(239 citation statements)

References 27 publications

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“…It has been observed that some variants might be more penetrant or have a larger effect because familial aggregation of disease is observed. 10,11 While locus heterogeneity makes it difficult to identify factors unambiguously influencing the KTCN phenotype, the replication for any particular gene is expected to be rare.…”

Section: Introductionmentioning

confidence: 99%

Variants in SKP1, PROB1, and IL17B genes at keratoconus 5q31.1–q35.3 susceptibility locus identified by whole-exome sequencing

et al. 2016

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Keratoconus (KTCN) is a protrusion and thinning of the cornea, resulting in impairment of visual function. The extreme genetic heterogeneity makes it difficult to discover factors unambiguously influencing the KTCN phenotype. In this study, we used whole-exome sequencing (WES) and Sanger sequencing to reduce the number of candidate genes at the 5q31.1-q35.3 locus and to prioritize other potentially relevant variants in an Ecuadorian family with KTCN. We applied WES in two affected KTCN individuals from the Ecuadorian family that showed a suggestive linkage between the KTCN phenotype and the 5q31.1-q35.3 locus. Putative variants identified by WES were further evaluated in this family using Sanger sequencing. Exome capture discovered a total of 173 rare (minor allele frequency o0.001 in control population) nonsynonymous variants in both affected individuals. Among them, 16 SNVs were selected for further evaluation. Segregation analysis revealed that variants c.475T4G in SKP1, c.671G4A in PROB1, and c.527G4A in IL17B in the 5q31.1-q35.3 linkage region, and c.850G4A in HKDC1 in the 10q22 locus completely segregated with the phenotype in the studied KTCN family. We demonstrate that a combination of various techniques significantly narrowed the studied genomic region and reduced the list of the putative exonic variants. Moreover, since this locus overlapped two other chromosomal regions previously recognized in distinct KTCN studies, our findings suggest that this 5q31.1-q35.3 locus might be linked with KTCN.

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Section: Introductionmentioning

confidence: 99%

Variants in SKP1, PROB1, and IL17B genes at keratoconus 5q31.1–q35.3 susceptibility locus identified by whole-exome sequencing

et al. 2016

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“…47 Concordance is also high among monozygotic twins and a greater similarity of phenotype is observed in monozygotic twin pairs implying that genetic factors are likely to have a key role in the disease phenotype. 48 KC has been associated with a wide range of systemic and ocular conditions, for example Leber congenital amaurosis, 49 anterior polar cataract, 50 Brittle cornea syndrome, 51,52 and with a 10-300-fold higher prevalence in individuals with Down syndrome. 53,54 Interestingly, individuals with connective tissue disorders such as Ehlers Danlos syndrome have a higher prevalence of KC.…”

Section: Geneticsmentioning

confidence: 99%

“…81 Of particular relevance, linkage analysis in combination with nextgeneration sequencing identified a heterozygous mutation in mir-184 in two families with dominant congenital cataract associated with a corneal phenotype that in some cases was consistent with KC. 50,82,83 To establish whether mutations in mir-184 were associated with KC, mir-184 was subsequently screened in a cohort of 780 KC patients. 84 Rare variants were identified in two (0.25%) patients, but the variants did not fully segregate with disease, suggesting that mir-184 variants are not a common cause of isolated KC.…”

Section: Geneticsmentioning

confidence: 99%

The pathogenesis of keratoconus

Davidson¹,

Hayes

Hardcastle³

et al. 2013

Eye

285

216

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Keratoconus (KC) is a common degenerative condition that frequently results in visual loss with an onset typically in early adulthood. It is the single most common reason for keratoplasty in the developed world. The cause and underlying pathological mechanism are unknown, but both environmental and genetic factors are thought to contribute to the development of the disease. Various strategies have been employed to address the gap in our understanding of this complex disease, with the expectation that over time more sophisticated therapies will be developed. In this review we summarise our current knowledge of the aetiology and risk factors associated with KC.

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“…Genome-wide linkage analysis of affected pedigrees has shown evidence of disease susceptibility genes mapping to several putative chromosomal loci. [48][49][50][51] …”

Section: Genetic Locimentioning

confidence: 99%

The Epidemiology and Etiology of Keratoconus

Gordon‐Shaag¹,

Millodot²,

Shneor³

2012

International Journal of Keratoconus and Ectatic Corneal Diseases

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Keratoconus is a noninflammatory disorder characterized by ectasia of the central or inferior portion of the cornea. This review presents the scant epidemiological information known to date and the factors believed to cause the development of the disease. They are the genetic factors for which evidence come from family studies, twin studies and genetic loci. There appears to be multiple genes causing a keratoconus phenotype with variable penetration. However, the genetic predisposition might not be enough; environmental factors, such as eye rubbing, atopy and UV exposure, may have a role in generating the disease.

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Mutation Altering the miR-184 Seed Region Causes Familial Keratoconus with Cataract

Cited by 239 publications

References 27 publications

Variants in SKP1, PROB1, and IL17B genes at keratoconus 5q31.1–q35.3 susceptibility locus identified by whole-exome sequencing

Variants in SKP1, PROB1, and IL17B genes at keratoconus 5q31.1–q35.3 susceptibility locus identified by whole-exome sequencing

The pathogenesis of keratoconus

The Epidemiology and Etiology of Keratoconus

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