Case-control genetic association study of fibullin-6 (FBLN6 or HMCN1) variants in age-related macular degeneration (AMD)

S A Fisher; A Rivera; L G Fritsche; C N Keilhauer; P Lichtner; T Meitinger; G Rudolph; B H E Weber

doi:10.1002/humu.20464

Case-control genetic association study of fibullin-6 (FBLN6 or HMCN1) variants in age-related macular degeneration (AMD)

S A Fisher, A Rivera, L G Fritsche, C N Keilhauer, P Lichtner, T Meitinger, G Rudolph, B H E Weber

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Abstract

This article reports a well-powered age,related macular degeneration (AMD) case-control association study in the HMCN1 gene, showing that common variants do not account for a substantial proportion of AMD cases. Thus, the consistent linkage peak observed by several genome-wide linkage scans within the 1q32 region is unlikely to be attributed to polymorphisms at the HMCN1 locus. In addition, the analysis provides comprehensive data suggesting that low-frequency variants encoding possible functional amino acid polymorphisms in the HMCN1 gene may not contribute substantially to disease, although HMCN1 mutations may still confer disease susceptibility in a small subset of patients. Interestingly, the HMCN1 p.Gln5346Arg mutation, which is thought to be a causal mutation in a large AMD pedigree segregating the disease as a single-gene trait, appears to occur in our control cohort as a low-frequency polymorphism with an allele frequency of approximately 0.0026

Original language	English
Pages (from-to)	406 - 413
Number of pages	8
Journal	Human Mutation
Volume	28
Issue number	4
DOIs	https://doi.org/10.1002/humu.20464
Publication status	Published - Apr 2007

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title = "Case-control genetic association study of fibullin-6 (FBLN6 or HMCN1) variants in age-related macular degeneration (AMD)",

abstract = "This article reports a well-powered age,related macular degeneration (AMD) case-control association study in the HMCN1 gene, showing that common variants do not account for a substantial proportion of AMD cases. Thus, the consistent linkage peak observed by several genome-wide linkage scans within the 1q32 region is unlikely to be attributed to polymorphisms at the HMCN1 locus. In addition, the analysis provides comprehensive data suggesting that low-frequency variants encoding possible functional amino acid polymorphisms in the HMCN1 gene may not contribute substantially to disease, although HMCN1 mutations may still confer disease susceptibility in a small subset of patients. Interestingly, the HMCN1 p.Gln5346Arg mutation, which is thought to be a causal mutation in a large AMD pedigree segregating the disease as a single-gene trait, appears to occur in our control cohort as a low-frequency polymorphism with an allele frequency of approximately 0.0026",

author = "Fisher, {S A} and A Rivera and Fritsche, {L G} and Keilhauer, {C N} and P Lichtner and T Meitinger and G Rudolph and Weber, {B H E}",

year = "2007",

month = apr,

doi = "10.1002/humu.20464",

language = "English",

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pages = "406 -- 413",

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T1 - Case-control genetic association study of fibullin-6 (FBLN6 or HMCN1) variants in age-related macular degeneration (AMD)

AU - Fisher, S A

AU - Rivera, A

AU - Fritsche, L G

AU - Keilhauer, C N

AU - Lichtner, P

AU - Meitinger, T

AU - Rudolph, G

AU - Weber, B H E

PY - 2007/4

Y1 - 2007/4

N2 - This article reports a well-powered age,related macular degeneration (AMD) case-control association study in the HMCN1 gene, showing that common variants do not account for a substantial proportion of AMD cases. Thus, the consistent linkage peak observed by several genome-wide linkage scans within the 1q32 region is unlikely to be attributed to polymorphisms at the HMCN1 locus. In addition, the analysis provides comprehensive data suggesting that low-frequency variants encoding possible functional amino acid polymorphisms in the HMCN1 gene may not contribute substantially to disease, although HMCN1 mutations may still confer disease susceptibility in a small subset of patients. Interestingly, the HMCN1 p.Gln5346Arg mutation, which is thought to be a causal mutation in a large AMD pedigree segregating the disease as a single-gene trait, appears to occur in our control cohort as a low-frequency polymorphism with an allele frequency of approximately 0.0026

AB - This article reports a well-powered age,related macular degeneration (AMD) case-control association study in the HMCN1 gene, showing that common variants do not account for a substantial proportion of AMD cases. Thus, the consistent linkage peak observed by several genome-wide linkage scans within the 1q32 region is unlikely to be attributed to polymorphisms at the HMCN1 locus. In addition, the analysis provides comprehensive data suggesting that low-frequency variants encoding possible functional amino acid polymorphisms in the HMCN1 gene may not contribute substantially to disease, although HMCN1 mutations may still confer disease susceptibility in a small subset of patients. Interestingly, the HMCN1 p.Gln5346Arg mutation, which is thought to be a causal mutation in a large AMD pedigree segregating the disease as a single-gene trait, appears to occur in our control cohort as a low-frequency polymorphism with an allele frequency of approximately 0.0026

U2 - 10.1002/humu.20464

DO - 10.1002/humu.20464

M3 - Article

VL - 28

SP - 406

EP - 413

JO - Human Mutation

JF - Human Mutation

IS - 4

ER -

Case-control genetic association study of fibullin-6 (FBLN6 or HMCN1) variants in age-related macular degeneration (AMD)

Abstract

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