Targeted next-generation sequencing analysis in Italian patients with keratoconus

Objective To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Subjects/methods Sixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups accor...

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Published inEye (London) Vol. 38; no. 13; pp. 2610 - 2618
Main Authors Lombardo, Marco, Camellin, Umberto, Gioia, Raffaella, Serrao, Sebastiano, Scorcia, Vincenzo, Roszkowska, Anna Maria, Lombardo, Giuseppe, Bertelli, Matteo, Medori, Maria Chiara, Alunni Fegatelli, Danilo, Vestri, Annarita, Mencucci, Rita, Schiano Lomoriello, Domenico
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 01.09.2024
Nature Publishing Group
Subjects
45/23
692/420/2489/144
692/499
Adolescent
Adult
Cornea
Diagnosis
Exons
Female
Filaggrin
Filaggrin Proteins
Genetic Association Studies
Genetic diversity
GTPase-Activating Proteins - genetics
Guanine Nucleotide Exchange Factors - genetics
High-Throughput Nucleotide Sequencing
Humans
Intermediate Filament Proteins - genetics
Italy
Keratoconus
Keratoconus - diagnosis
Keratoconus - genetics
Laboratory Medicine
Male
Medicine
Medicine & Public Health
Middle Aged
Mutation
Next-generation sequencing
Ophthalmology
Pharmaceutical Sciences/Technology
Phenotypes
Population studies
Risk factors
Sequence analysis
Surgery
Surgical Oncology
Transcription Factors
Young Adult
Italy
Online AccessGet full text
ISSN0950-222X
1476-5454
1476-5454
DOI10.1038/s41433-024-03090-5

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Abstract Objective To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Subjects/methods Sixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms. Result The targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease. Conclusions Targeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.
AbstractList To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Sixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms. The targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease. Targeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.
Objective To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Subjects/methods Sixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms. Result The targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease. Conclusions Targeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.
To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC).OBJECTIVETo report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC).Sixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms.SUBJECTS/METHODSSixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms.The targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease.RESULTThe targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease.Targeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.CONCLUSIONSTargeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.
ObjectiveTo report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC).Subjects/methodsSixty-four patients with a confirmed diagnosis of KC were enrolled in this genetic association study. Patients were classified into two study groups according to whether they had a confirmed diagnosis of progressive or stable KC. A purpose-developed Next Generation Sequencing (NGS) panel was used to identify and analyse the coding exons and flanking exon/intron boundaries of 26 genes known to be associated with KC and corneal dystrophies. Interpretation of the pathogenic significance of variants was performed using in silico predictive algorithms.ResultThe targeted NGS research identified a total of 167 allelic variants of 22 genes in the study population; twenty-four patients had stable keratoconus (n. 54 variants) and forty patients had progressive disease (n. 113 variants). We identified genetic variants of certain pathogenic significance in five patients with progressive KC; in addition, eight novel genetic variants were found in eight patients with progressive KC. Mutations of FLG, LOXHD1, ZNF469, and DOCK9 genes were twice more frequently identified in patients with progressive than stable disease. Filaggrin gene variants were found in 49 patients (76% of total), of whom 32 patients (80% of progressive KC group) had progressive disease.ConclusionsTargeted NGS research provided new insights into the causative effect of candidate genes in the clinical phenotype of keratoconus. Filaggrin mutations were found to represent a genetic risk factor for development of progressive disease in Italy.
Author Gioia, Raffaella
Bertelli, Matteo
Alunni Fegatelli, Danilo
Schiano Lomoriello, Domenico
Lombardo, Marco
Camellin, Umberto
Scorcia, Vincenzo
Mencucci, Rita
Roszkowska, Anna Maria
Lombardo, Giuseppe
Medori, Maria Chiara
Serrao, Sebastiano
Vestri, Annarita
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SSID ssj0014770
Score 2.4097507
Snippet Objective To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Subjects/methods Sixty-four...
To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC). Sixty-four patients with a confirmed...
ObjectiveTo report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC).Subjects/methodsSixty-four...
To report variants in 26 candidate genes and describe the clinical features of Italian patients with keratoconus (KC).OBJECTIVETo report variants in 26...
SourceID pubmedcentral
proquest
pubmed
crossref
springer
SourceType Open Access Repository
Aggregation Database
Index Database
Enrichment Source
Publisher
StartPage 2610
SubjectTerms 45/23
692/420/2489/144
692/499
Adolescent
Adult
Cornea
Diagnosis
Exons
Female
Filaggrin
Filaggrin Proteins
Genetic Association Studies
Genetic diversity
GTPase-Activating Proteins - genetics
Guanine Nucleotide Exchange Factors - genetics
High-Throughput Nucleotide Sequencing
Humans
Intermediate Filament Proteins - genetics
Italy
Keratoconus
Keratoconus - diagnosis
Keratoconus - genetics
Laboratory Medicine
Male
Medicine
Medicine & Public Health
Middle Aged
Mutation
Next-generation sequencing
Ophthalmology
Pharmaceutical Sciences/Technology
Phenotypes
Population studies
Risk factors
Sequence analysis
Surgery
Surgical Oncology
Transcription Factors
Young Adult
Title Targeted next-generation sequencing analysis in Italian patients with keratoconus
URI https://link.springer.com/article/10.1038/s41433-024-03090-5
https://www.ncbi.nlm.nih.gov/pubmed/38684849
https://www.proquest.com/docview/3102223870
https://www.proquest.com/docview/3049720164
https://pubmed.ncbi.nlm.nih.gov/PMC11383948
Volume 38
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