Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis

PURPOSE: Leber congenital amaurosis (LCA) is one of the most common causes of hereditary blindness in infants. To date, mutations in 13 known genes and at two other loci have been implicated in LCA causation. An examination of the known genes highlights several processes which, when defective, cause...

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Autores principales: Ramprasad, Vedam Lakshmi, Soumittra, Nagasamy, Nancarrow, Derek, Sen, Parveen, McKibbin, Martin, Williams, Grange A, Arokiasamy, Tharigopala, Lakshmipathy, Praveena, Inglehearn, Chris F, Kumaramanickavel, Govindasamy
Formato: Texto
Lenguaje:English
Publicado: Molecular Vision 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2268850/
https://www.ncbi.nlm.nih.gov/pubmed/18334959
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author Ramprasad, Vedam Lakshmi
Soumittra, Nagasamy
Nancarrow, Derek
Sen, Parveen
McKibbin, Martin
Williams, Grange A
Arokiasamy, Tharigopala
Lakshmipathy, Praveena
Inglehearn, Chris F
Kumaramanickavel, Govindasamy
author_facet Ramprasad, Vedam Lakshmi
Soumittra, Nagasamy
Nancarrow, Derek
Sen, Parveen
McKibbin, Martin
Williams, Grange A
Arokiasamy, Tharigopala
Lakshmipathy, Praveena
Inglehearn, Chris F
Kumaramanickavel, Govindasamy
author_sort Ramprasad, Vedam Lakshmi
collection PubMed
description PURPOSE: Leber congenital amaurosis (LCA) is one of the most common causes of hereditary blindness in infants. To date, mutations in 13 known genes and at two other loci have been implicated in LCA causation. An examination of the known genes highlights several processes which, when defective, cause LCA, including photoreceptor development and maintenance, phototransduction, vitamin A metabolism, and protein trafficking. In addition, it has been known for some time that defects in sensory cilia can cause syndromes involving hereditary blindness. More recently evidence has come to light that non-syndromic LCA can also be a “ciliopathy.” METHODS: Here we present a homozygosity mapping analysis in a consanguineous sibship that led to the identification of a mutation in the recently discovered LCA5 gene. Homozygosity mapping was done using Affymetrix 10K Xba I Gene Chip and a 24.5cM region on chromosome 6 (6q12- q16.3) was identified to be significantly homozygous. The LCA5 gene on this region was sequenced and cDNA sequencing also done to characterize the mutation. RESULTS: A c.955G>A missense mutation in the last base of exon 6 causing disruption of the splice donor site was identified in both the affected sibs. Since there is a second consensus splice donor sequence 5 bp into the adjacent intron, this mutation results in a transcript with a 5 bp insertion of intronic sequence, leading to a frameshift and premature truncation. CONCLUSIONS: We report a missense mutation functionally altering the splice donor site and leading to a truncated protein. This is the second report of LCA5 mutations causing LCA. It may also be significant that one affected child died at eleven months of age due to asphyxia during sleep. To date the only phenotype unambiguously associated with mutations in this gene is LCA. However the LCA5 gene is known to be expressed in nasopharynx, trachea and lungs and was originally identified in the proteome of bronchial epithelium ciliary axonemes. The cause of death in this child may therefore imply that LCA5 mutations can in fact cause a wider spectrum of phenotypes including respiratory disease.
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spelling pubmed-22688502008-03-20 Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis Ramprasad, Vedam Lakshmi Soumittra, Nagasamy Nancarrow, Derek Sen, Parveen McKibbin, Martin Williams, Grange A Arokiasamy, Tharigopala Lakshmipathy, Praveena Inglehearn, Chris F Kumaramanickavel, Govindasamy Mol Vis Research Article PURPOSE: Leber congenital amaurosis (LCA) is one of the most common causes of hereditary blindness in infants. To date, mutations in 13 known genes and at two other loci have been implicated in LCA causation. An examination of the known genes highlights several processes which, when defective, cause LCA, including photoreceptor development and maintenance, phototransduction, vitamin A metabolism, and protein trafficking. In addition, it has been known for some time that defects in sensory cilia can cause syndromes involving hereditary blindness. More recently evidence has come to light that non-syndromic LCA can also be a “ciliopathy.” METHODS: Here we present a homozygosity mapping analysis in a consanguineous sibship that led to the identification of a mutation in the recently discovered LCA5 gene. Homozygosity mapping was done using Affymetrix 10K Xba I Gene Chip and a 24.5cM region on chromosome 6 (6q12- q16.3) was identified to be significantly homozygous. The LCA5 gene on this region was sequenced and cDNA sequencing also done to characterize the mutation. RESULTS: A c.955G>A missense mutation in the last base of exon 6 causing disruption of the splice donor site was identified in both the affected sibs. Since there is a second consensus splice donor sequence 5 bp into the adjacent intron, this mutation results in a transcript with a 5 bp insertion of intronic sequence, leading to a frameshift and premature truncation. CONCLUSIONS: We report a missense mutation functionally altering the splice donor site and leading to a truncated protein. This is the second report of LCA5 mutations causing LCA. It may also be significant that one affected child died at eleven months of age due to asphyxia during sleep. To date the only phenotype unambiguously associated with mutations in this gene is LCA. However the LCA5 gene is known to be expressed in nasopharynx, trachea and lungs and was originally identified in the proteome of bronchial epithelium ciliary axonemes. The cause of death in this child may therefore imply that LCA5 mutations can in fact cause a wider spectrum of phenotypes including respiratory disease. Molecular Vision 2008-03-10 /pmc/articles/PMC2268850/ /pubmed/18334959 Text en http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Ramprasad, Vedam Lakshmi
Soumittra, Nagasamy
Nancarrow, Derek
Sen, Parveen
McKibbin, Martin
Williams, Grange A
Arokiasamy, Tharigopala
Lakshmipathy, Praveena
Inglehearn, Chris F
Kumaramanickavel, Govindasamy
Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title_full Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title_fullStr Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title_full_unstemmed Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title_short Identification of a novel splice-site mutation in the Lebercilin (LCA5) gene causing Leber congenital amaurosis
title_sort identification of a novel splice-site mutation in the lebercilin (lca5) gene causing leber congenital amaurosis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2268850/
https://www.ncbi.nlm.nih.gov/pubmed/18334959
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