Exploring the Genetic Landscape of Retinal Diseases in North-Western Pakistan Reveals a High Degree of Autozygosity and a Prevalent Founder Mutation in ABCA4

Rehman, Atta Ur; Peter, Virginie G.; Quinodoz, Mathieu; Rashid, Abdur; Khan, Syed Akhtar; Superti‐Furga, Andrea; Rivolta, Carlo

doi:10.3390/genes11010012

Cited by 11 publications

(16 citation statements)

References 43 publications

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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: 78%

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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Section: Irds—target Panels and Whole Exome Studiesmentioning

confidence: 78%

Next-Generation Sequencing Applications for Inherited Retinal Diseases

Dockery

Whelan

Humphries

et al. 2021

IJMS

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“…The same was true for the two other studies, where the presence of false-positive heterozygous genotypes was combined with the relatively short size of ROHs and/or the presence of a limited number of identifiable genotypes. In addition, AutoMap enabled the detection of new variants in a number of genes that were already associated with Mendelian conditions [35][36][37] . In conclusion, AutoMap is a reliable tool that can predict ROHs with high specificity and sensitivity, in less than a minute, even from VCF files derived from noisy exome sequencing data.…”

Section: Resultsmentioning

confidence: 99%

AutoMap is a high performance homozygosity mapping tool using next-generation sequencing data

Quinodoz

Peter

Bedoni³

et al. 2021

Nat Commun

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Homozygosity mapping is a powerful method for identifying mutations in patients with recessive conditions, especially in consanguineous families or isolated populations. Historically, it has been used in conjunction with genotypes from highly polymorphic markers, such as DNA microsatellites or common SNPs. Traditional software performs rather poorly with data from Whole Exome Sequencing (WES) and Whole Genome Sequencing (WGS), which are now extensively used in medical genetics. We develop AutoMap, a tool that is both web-based or downloadable, to allow performing homozygosity mapping directly on VCF (Variant Call Format) calls from WES or WGS projects. Following a training step on WES data from 26 consanguineous families and a validation procedure on a matched cohort, our method shows higher overall performances when compared with eight existing tools. Most importantly, when tested on real cases with negative molecular diagnosis from an internal set, AutoMap detects three gene-disease and multiple variant-disease associations that were previously unrecognized, projecting clear benefits for both molecular diagnosis and research activities in medical genetics.

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“…The rationale for this method is that unaffected parents who have some degree of kinship, belong to an ethnic group with high endogamy or are from a geographical isolate, could be heterozygotes for the same recessive mutation from a common ancestor. This mutation, which at the population level possibly will even be infrequent, can be brought to homozygosity since consanguinity can cause disease in these parents' children 23,24 . This feature makes the Iranian gene pool one of the richest resources for genetic investigations.…”

Section: Discussionmentioning

confidence: 99%

Whole exome sequencing and homozygosity mapping reveals genetic defects in consanguineous Iranian families with inherited retinal dystrophies

Salmaninejad

Bedoni

Ravesh

et al. 2020

Sci Rep

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Inherited retinal dystrophies (IRDs), displaying pronounced genetic and clinical heterogeneity, comprise of a broad range of diseases characterized by progressive retinal cell death and gradual loss of vision. By the combined use of whole exome sequencing (WES), SNP-array and WES-based homozygosity mapping, as well as directed DNA sequencing (Sanger), we have identified nine pathogenic variants in six genes (ABCA4, RPE65, MERTK, USH2A, SPATA7, TULP1) in 10 consanguineous Iranian families. Six of the nine identified variants were novel, including a putative founder mutation in ABCA4 (c.3260A>G, p.Glu1087Gly), detected in two families from Northeastern Iran. Our findings provide additional information to the molecular pathology of IRDs in Iran, hopefully contributing to better genetic counselling and patient management in the respective families from this country.

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Exploring the Genetic Landscape of Retinal Diseases in North-Western Pakistan Reveals a High Degree of Autozygosity and a Prevalent Founder Mutation in ABCA4

Cited by 11 publications

References 43 publications

Next-Generation Sequencing Applications for Inherited Retinal Diseases

Next-Generation Sequencing Applications for Inherited Retinal Diseases

AutoMap is a high performance homozygosity mapping tool using next-generation sequencing data

Whole exome sequencing and homozygosity mapping reveals genetic defects in consanguineous Iranian families with inherited retinal dystrophies

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