A high prevalence of biallelic<i>RPE65</i>mutations in Costa Rican children with Leber congenital amaurosis and early-onset retinal dystrophy

Glen, W. Bailey; Peterseim, Mae Millicent W.; Badilla, Ramses; Znoyko, Iya; Bourg, Andre; Wilson, Robert; Hardiman, Gary; Wolff, Daynna J.; Martínez, José Belmonte

doi:10.1080/13816810.2019.1582069

Cited by 9 publications

(11 citation statements)

References 42 publications

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“…A total of 212 pathogenic variants in RPE65 have been reported to date (HGMD, [17]), of which the majority are missense (54.71%), followed by nonsense-frameshift (32.54%) and splice site variants (12%). A similar frequency of the type of mutation was observed in our cohort (57%, 28% and 11%, respectively); thus, our cohort is representative of the first described in LCA patients from India [15] and Central America [45], being related to more severe phenotypes. Interestingly, p.(Ile98Hisfs*26) seems to represent a founder mutation in our cohort with all the carriers families sharing a common haplotype.…”

Section: Genotype-phenotype Correlationsupporting

confidence: 85%

“…By contrast, the most common alleles found in our cohort were p.(Ile98Hisfs*26, p.(Pro111Ser) and p.(Gly187Glu). The p.(Ile98Hisfs*26) variant was first described in LCA patients from India [15] and Central America [45], being related to more severe phenotypes. Interestingly, p.(Ile98Hisfs*26) seems to represent a founder mutation in our cohort with all the carriers families sharing a common haplotype.…”

Section: Discussionmentioning

confidence: 99%

“…Interestingly, p.(Ile98Hisfs*26) seems to represent a founder mutation in our cohort with all the carriers families sharing a common haplotype. Due to the historical influence of the Spanish ancestry in Central and South America populations, this finding could be related to the enrichment of this rare variant in the Latino cohort of GnomAD and to its increased frequency in LCA patients from Costa Rica where this variant was reported as a recurrent mutation [45]. The variant p.(Pro111Ser), which is carried by 3 of our families, were first described in our cohort of patients, as recently we reported [25].…”

Section: Discussionmentioning

confidence: 99%

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RPE65-related retinal dystrophy: mutational and phenotypic spectrum in 45 affected patients

López‐Rodríguez

Lantero

Blanco‐Kelly

et al. 2021

Preprint

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BackgroundBiallelic pathogenic RPE65 variants are related to a spectrum of clinically overlapping inherited retinal dystrophies (IRD). Most affected individuals show a severe progression, with 50% of patients legally blind by 20 years of age. A better knowledge of the mutational spectrum and the phenotype-genotype correlation in RPE65-related IRD is needed.MethodsForty-five affected subjects from 27 unrelated families with a clinical diagnosis of RPE65-related IRD were included. Clinical evaluation consisted on self-reported ophthalmological history and objective ophthalmological examination. Patients’ genotype was classified accordingly to variant class (truncating or missense) or to variant location at different protein domains. Main phenotypic outcome was age at onset (AAO) of the symptomatic disease and a Kaplan–Meier analysis of disease symptom event-free survival was performed.ResultsTwenty-nine different RPE65 variants were identified in our cohort, 7 of them novel. Most frequent variants were p.(Ile98Hisfs*26), p.(Pro111Ser) and p.(Gly187Glu) accounting for the 24% of the detected alleles. Patients carrying two missense alleles showed a later disease onset than those with 1 or 2 truncating variants (Log Rank test p<0.05). While the 60% of patients carrying a missense/missense genotype presented symptoms before or at the first year of life, almost all patients with at least 1 truncating allele (91%) had an AAO ≤1 year (p<0.05).ConclusionOur findings suggest an association between the type of the RPE65 carried variant and the AAO. Thus, our results provide useful data on RPE65-associated IRD phenotypes which may help to improve clinical and therapeutic management of these patients.

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Section: Genotype-phenotype Correlationsupporting

confidence: 85%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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RPE65-related retinal dystrophy: mutational and phenotypic spectrum in 45 affected patients

López‐Rodríguez

Lantero

Blanco‐Kelly

et al. 2021

Preprint

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“…Similarly, EYS gene variants were found to be causative in 51% of a RP cohort from Japan [ 36 ]. This discovery is not unique, as several other parallel studies have revealed similar founder mutations in their target populations, for example, Belgium, RAX2 [ 37 ]; Costa Rica, RPE65 [ 38 ]; Finland, CERKL [ 39 ]; Japan, EYS [ 36 ]; Spain, RP1 [ 40 ] and ABCA4 [ 41 ]; Jewish community in Caucasia, PDE6B [ 42 ]; Pakistan, ABCA4 and NMNAT1 [ 43 ]; Guyana, BBS9 [ 44 ]; and Faroe Islands, MERTK [ 45 ]. The enrichment of these variants, several of which are large structural variants, emphasises the value of population-specific TS panels to target and detect mutations and mutational breakpoints that may be missed by commercial generic gene panel sequencing or even WES.…”

Section: Irds—target Panels and Whole Exome Studiesmentioning

confidence: 66%

Next-Generation Sequencing Applications for Inherited Retinal Diseases

Dockery

Whelan

Humphries

et al. 2021

IJMS

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Inherited retinal diseases (IRDs) represent a collection of phenotypically and genetically diverse conditions. IRDs phenotype(s) can be isolated to the eye or can involve multiple tissues. These conditions are associated with diverse forms of inheritance, and variants within the same gene often can be associated with multiple distinct phenotypes. Such aspects of the IRDs highlight the difficulty met when establishing a genetic diagnosis in patients. Here we provide an overview of cutting-edge next-generation sequencing techniques and strategies currently in use to maximise the effectivity of IRD gene screening. These techniques have helped researchers globally to find elusive causes of IRDs, including copy number variants, structural variants, new IRD genes and deep intronic variants, among others. Resolving a genetic diagnosis with thorough testing enables a more accurate diagnosis and more informed prognosis and should also provide information on inheritance patterns which may be of particular interest to patients of a child-bearing age. Given that IRDs are heritable conditions, genetic counselling may be offered to help inform family planning, carrier testing and prenatal screening. Additionally, a verified genetic diagnosis may enable access to appropriate clinical trials or approved medications that may be available for the condition.

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“…2,6,75 Over 100 mutations are associated with the pathogenesis of arLCA, 2,6,75-78 RP. 6,[75][76][77] adult onset vitelliform macular dystrophy 79 and CRD. 80 Although it may produce both adRP and arRP, it is mostly associated with arRP.…”

Section: Rpe65 Genementioning

confidence: 99%

Recent Developments on the major genes involved in retinitis pigmentosa

A¹,

D²,

A³

et al. 2020

IJOOO

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Retinitis pigmentosa (RP) is a common retinal dystrophy that affects millions of individuals, of both sexes, worldwide. The age of onset and the phenotypic characteristics vary between patients of different ethnicities. It may be syndromic when it coexists with several syndromes, like Usher syndrome, or nonsyndromic. It follows autosomal dominant, autosomal recessive or X-linked inheritance. RP is genetically heterogeneous with, approximately, one hundred genes identified to date. The present mini review includes articles about the pathogenesis of syndromic and non-syndromic RP. Eighty-seven papers written in English and published in the last decade, about the pathogenesis of RP were reviewed and analyzed in order to summarize and highlight the major genes implicated in RP. We identified more than 80 genes associated with syndromic and 30 genes with non-syndromic RP. Among them RHO and RPGR, followed by PRPH2, PRPF31 and RP2 are the major genes involved in RP.

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A high prevalence of biallelicRPE65mutations in Costa Rican children with Leber congenital amaurosis and early-onset retinal dystrophy

Cited by 9 publications

References 42 publications

RPE65-related retinal dystrophy: mutational and phenotypic spectrum in 45 affected patients

RPE65-related retinal dystrophy: mutational and phenotypic spectrum in 45 affected patients

Next-Generation Sequencing Applications for Inherited Retinal Diseases

Recent Developments on the major genes involved in retinitis pigmentosa

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