A Novel Recurrent 200 kb CRYL1 Deletion Underlies DFNB1A Hearing Loss in Patients from Northwestern Spain.

Cifuentes, Guadalupe A; Diñeiro, Marta; Huete, Alicia R; Capín, Raquel; Santiago, Adrián; Vargas, Alberto A R; Carrero, Dido; Martínez, Esther López; Aguiar, Beatriz; Fischer, Anja; Rad, Roland; Costales, María; Cabanillas, Rubén; Cadiñanos, Juan

doi:10.3390/genes16060670

Benutzer: Gast

Institut für Molekulare Onkologie und Funktionelle Genomik (Prof. Rad)

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Titel:: A Novel Recurrent 200 kb CRYL1 Deletion Underlies DFNB1A Hearing Loss in Patients from Northwestern Spain.
Dokumenttyp:: Journal Article
Autor(en):: Cifuentes, Guadalupe A; Diñeiro, Marta; Huete, Alicia R; Capín, Raquel; Santiago, Adrián; Vargas, Alberto A R; Carrero, Dido; Martínez, Esther López; Aguiar, Beatriz; Fischer, Anja; Rad, Roland; Costales, María; Cabanillas, Rubén; Cadiñanos, Juan
Abstract:: BACKGROUND/OBJECTIVES: Pathogenic recessive GJB2 variants are the main genetic cause of non-syndromic sensorineural hearing loss. However, following GJB2 testing, a significant proportion of deaf patients are only found to be heterozygous carriers of pathogenic GJB2 alleles. Five large deletions not affecting GJB2 but encompassing a minimal common 62 kb region within the neighbouring CRYL1 gene have been described to cause loss of cis GJB2 expression and, as a result, produce hearing loss when in trans with pathogenic GJB2 variants. We describe the identification and characterization of a novel deletion of this type in deaf patients from northwestern Spain. METHODS: We used panel NGS sequencing to detect the deletion, MLPA to validate it, whole-genome sequencing to map its breakpoints, PCR + Sanger sequencing to finely characterize it and triple-primer PCR to screen for it. RESULTS: We identified a novel 200 kb deletion spanning the whole CRYL1 gene in two unrelated deaf patients from Asturias (in northwestern Spain) who were heterozygous for the pathogenic GJB2 c.35delG variant. Although the large deletion was absent from gnomAD v4.1.0 and 2052 local control alleles, screening for it in 20 additional deaf carriers of monoallelic pathogenic GJB2 variants detected it in another patient from Galicia (also in northwestern Spain). The novel deletion, termed del(200 kb)insATTATA, explained hearing loss in 3/43 (7%) deaf patients from our cohort that were otherwise heterozygous for pathogenic GJB2 variants. CONCLUSIONS: This work highlights the importance of comprehensively testing all genomic regions known to be clinically relevant for a given genetic condition, including thorough CRYL1 CNV screening for DFNB1A diagnostics. «
BACKGROUND/OBJECTIVES: Pathogenic recessive GJB2 variants are the main genetic cause of non-syndromic sensorineural hearing loss. However, following GJB2 testing, a significant proportion of deaf patients are only found to be heterozygous carriers of pathogenic GJB2 alleles. Five large deletions not affecting GJB2 but encompassing a minimal common 62 kb region within the neighbouring CRYL1 gene have been described to cause loss of cis GJB2 expression and, as a result, produce hearing loss when i... »
Zeitschriftentitel:: Genes (Basel)
Jahr:: 2025
Band / Volume:: 16
Heft / Issue:: 6
Volltext / DOI:: doi:10.3390/genes16060670
PubMed:: http://view.ncbi.nlm.nih.gov/pubmed/40565562
Print-ISSN:: 2073-4425
TUM Einrichtung:: Professur für Molekulare Onkologie und Funktionelle Genomik (Prof. Rad)
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