Complex inheritance of ABCA4 disease: four mutations in a family with multiple macular phenotypes
Over 800 mutations in the ABCA4 gene cause autosomal recessive Stargardt disease. Due to extensive genetic heterogeneity, observed variant-associated phenotypes can manifest tremendous variability of expression. Furthermore, the high carrier frequency of pathogenic ABCA4 alleles in the general popul...
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Veröffentlicht in: | Human genetics 2016-01, Vol.135 (1), p.9-19 |
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Sprache: | eng |
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Zusammenfassung: | Over 800 mutations in the
ABCA4
gene cause autosomal recessive Stargardt disease. Due to extensive genetic heterogeneity, observed variant-associated phenotypes can manifest tremendous variability of expression. Furthermore, the high carrier frequency of pathogenic
ABCA4
alleles in the general population (~1:20) often results in pseudo-dominant inheritance patterns further complicating the diagnosis and characterization of affected individuals. This study describes a genotype/phenotype analysis of an unusual family with multiple macular disease phenotypes spanning across two generations and segregating four distinct
ABCA4
mutant alleles. Complete sequencing of
ABCA4
discovered two known missense mutations, p.C54Y and p.G1961E. Array comparative genomic hybridization revealed a large novel deletion combined with a small insertion, c.6148-698_c.6670del/insTGTGCACCTCCCTAG, and complete sequencing of the entire
ABCA4
genomic locus uncovered a new deep intronic variant, c.302+68C>T. Patients with the p.G1961E mutation had the mildest, confined maculopathy phenotype with peripheral flecks while those with all other mutant allele combinations exhibited a more advanced stage of generalized retinal and choriocapillaris atrophy. This family epitomizes the clinical and genetic complexity of
ABCA4
-associated diseases. It contained variants from all classes of mutations, in the coding region, deep intronic, both single nucleotide variants and copy number variants that accounted for varying phenotypes segregating in an apparent dominant fashion. Unequivocally defining disease-associated alleles in the
ABCA4
locus requires a multifaceted approach that includes advanced mutation detection methods and a thorough analysis of clinical phenotypes. |
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ISSN: | 0340-6717 1432-1203 |
DOI: | 10.1007/s00439-015-1605-y |