Association between a common missense variant in LOXL3 gene and the risk of non‐syndromic cleft palate

Association between a common missense variant in LOXL3 gene and the risk of non‐syndromic cleft palate

ABSTRACT To investigate possible association between functional common variants in the lysyl oxidase like 3 gene and non‐syndromic cleft palate we selected a common missense variant p.Ile615Phe (rs17010021), which was predicted to have a probably damaging effect on the lysyl oxidase like 3 enzyme. W...

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Veröffentlicht in:Congenital anomalies 2018-07, Vol.58 (4), p.136-140
Hauptverfasser: Khan, Mohammad Faisal J., Little, Julian, Mossey, Peter A., Steegers‐Theunissen, Régine P.M., Bonsi, Martina, Bassi Andreasi, Rita, Rubini, Michele
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Sprache:eng
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Cleft lip/palate
cleft palate
Congenital anomalies
Etiology
Genotypes
Heterozygotes
Homozygotes
Infants
LOXL3 gene
Lysyl oxidase
lysyl oxidase like 3
missense variant
non‐syndromic
Oxidase
Parents
Phenotypes
Regression analysis
Risk assessment
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container_end_page 140
container_issue 4
container_start_page 136
container_title Congenital anomalies
container_volume 58
creator Khan, Mohammad Faisal J.
Little, Julian
Mossey, Peter A.
Steegers‐Theunissen, Régine P.M.
Bonsi, Martina
Bassi Andreasi, Rita
Rubini, Michele
description ABSTRACT To investigate possible association between functional common variants in the lysyl oxidase like 3 gene and non‐syndromic cleft palate we selected a common missense variant p.Ile615Phe (rs17010021), which was predicted to have a probably damaging effect on the lysyl oxidase like 3 enzyme. We genotyped 258 non‐syndromic cleft palate case‐parent triads of European origin and tested genetic association using the transmission disequilibrium test and log‐linear regression analyses of genotypic relative risks and of parent‐of‐origin effects. The observed genotype frequency in parents was in Hardy–Weinberg equilibrium. Compared with wild‐type Ile/Ile homozygotes, the relative risks for Phe/Phe homozygote infants was 6.87 (P value 3.0 × 10−3), while that for Ile/Phe heterozygotes was not significant. Assuming an autosomal recessive model, the relative risks for Phe/Phe genotype resulted 10.54 (P value 2.9 × 10−5), with a 3.6% population attributable risk. No parent‐of‐origin effect was observed. The identification in lysyl oxidase like 3 of a missense variant which under a recessive model associates with 10‐fold increased risk of non‐syndromic cleft palate supports the hypothesis that the genetic etiology of this congenital anomaly includes relatively uncommon recessive variants with moderate penetrance and located in genes which are also involved in syndromes that include cleft palate as part of the phenotype. Our findings require functional validation and replication in a larger independent genetic association study.
doi_str_mv 10.1111/cga.12288
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We genotyped 258 non‐syndromic cleft palate case‐parent triads of European origin and tested genetic association using the transmission disequilibrium test and log‐linear regression analyses of genotypic relative risks and of parent‐of‐origin effects. The observed genotype frequency in parents was in Hardy–Weinberg equilibrium. Compared with wild‐type Ile/Ile homozygotes, the relative risks for Phe/Phe homozygote infants was 6.87 (P value 3.0 × 10−3), while that for Ile/Phe heterozygotes was not significant. Assuming an autosomal recessive model, the relative risks for Phe/Phe genotype resulted 10.54 (P value 2.9 × 10−5), with a 3.6% population attributable risk. No parent‐of‐origin effect was observed. The identification in lysyl oxidase like 3 of a missense variant which under a recessive model associates with 10‐fold increased risk of non‐syndromic cleft palate supports the hypothesis that the genetic etiology of this congenital anomaly includes relatively uncommon recessive variants with moderate penetrance and located in genes which are also involved in syndromes that include cleft palate as part of the phenotype. 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We genotyped 258 non‐syndromic cleft palate case‐parent triads of European origin and tested genetic association using the transmission disequilibrium test and log‐linear regression analyses of genotypic relative risks and of parent‐of‐origin effects. The observed genotype frequency in parents was in Hardy–Weinberg equilibrium. Compared with wild‐type Ile/Ile homozygotes, the relative risks for Phe/Phe homozygote infants was 6.87 (P value 3.0 × 10−3), while that for Ile/Phe heterozygotes was not significant. Assuming an autosomal recessive model, the relative risks for Phe/Phe genotype resulted 10.54 (P value 2.9 × 10−5), with a 3.6% population attributable risk. No parent‐of‐origin effect was observed. The identification in lysyl oxidase like 3 of a missense variant which under a recessive model associates with 10‐fold increased risk of non‐syndromic cleft palate supports the hypothesis that the genetic etiology of this congenital anomaly includes relatively uncommon recessive variants with moderate penetrance and located in genes which are also involved in syndromes that include cleft palate as part of the phenotype. 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ispartof Congenital anomalies, 2018-07, Vol.58 (4), p.136-140
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subjects Cleft lip/palate
cleft palate
Congenital anomalies
Etiology
Genotypes
Heterozygotes
Homozygotes
Infants
LOXL3 gene
Lysyl oxidase
lysyl oxidase like 3
missense variant
non‐syndromic
Oxidase
Parents
Phenotypes
Regression analysis
Risk assessment
title Association between a common missense variant in LOXL3 gene and the risk of non‐syndromic cleft palate
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