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Analysis of a biomarker for Wegener's granulomatosis

Summary This molecular epidemiology study integrated questionnaire and genotype information to examine a disease susceptibility hypothesis. The study was based on a previously reported association demonstrated between a single nucleotide polymorphism (SNP) identified as A‐564G within the promoter of...

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Published in:	International journal of immunogenetics 2005-08, Vol.32 (4), p.237-243
Main Authors:	Cooley, P., Taylor, K. H., Czika, W., Seifer, C., Taylor, J. F.
Format:	Article
Language:	English
Subjects:	Autoimmune Diseases - epidemiology Case-Control Studies Demography Female Gene Frequency - genetics Genetic Markers - genetics Genetic Predisposition to Disease - genetics Granulomatosis with Polyangiitis - diagnosis Granulomatosis with Polyangiitis - genetics Haplotypes - genetics Humans Male Myeloblastin Polymorphism, Single Nucleotide - genetics Prevalence Promoter Regions, Genetic - genetics Serine Endopeptidases - genetics Surveys and Questionnaires
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container_title	International journal of immunogenetics
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creator	Cooley, P. Taylor, K. H. Czika, W. Seifer, C. Taylor, J. F.
description	Summary This molecular epidemiology study integrated questionnaire and genotype information to examine a disease susceptibility hypothesis. The study was based on a previously reported association demonstrated between a single nucleotide polymorphism (SNP) identified as A‐564G within the promoter of the proteinase‐3 gene (PRTN3) and the autoimmune disease Wegener's granulomatosis (WG). To further examine the strength of this association, we employed a family‐based design in which the inheritance of alternate alleles could be ascertained from the parents of affected and unaffected progeny. Genotype information for the study participants was derived from DNA samples from participants who collected buccal cells using a harvesting method that was non‐invasive and self‐administered. A brief questionnaire captured demographic data on the participants, the family relationships between participants, and the prevalence of autoimmune disease among family members. Samples were obtained on 132 individuals representing 43 WG cases and 89 unaffected controls. Thirty‐four nuclear families containing at least one unaffected sibling or parent of a WG case were represented in this sample. We found no evidence for an association between A‐564G and the likelihood of a WG diagnosis. We examined five additional SNPs and a sixth SNP haplotype within the PRTN3 promoter region in a family‐based association analysis and found no evidence that mutations within PRTN3 are associated with WG diagnosis.
doi_str_mv	10.1111/j.1744-313X.2005.00519.x
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A brief questionnaire captured demographic data on the participants, the family relationships between participants, and the prevalence of autoimmune disease among family members. Samples were obtained on 132 individuals representing 43 WG cases and 89 unaffected controls. Thirty‐four nuclear families containing at least one unaffected sibling or parent of a WG case were represented in this sample. We found no evidence for an association between A‐564G and the likelihood of a WG diagnosis. 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H.</creatorcontrib><creatorcontrib>Czika, W.</creatorcontrib><creatorcontrib>Seifer, C.</creatorcontrib><creatorcontrib>Taylor, J. F.</creatorcontrib><title>Analysis of a biomarker for Wegener's granulomatosis</title><title>International journal of immunogenetics</title><addtitle>Int J Immunogenet</addtitle><description>Summary This molecular epidemiology study integrated questionnaire and genotype information to examine a disease susceptibility hypothesis. The study was based on a previously reported association demonstrated between a single nucleotide polymorphism (SNP) identified as A‐564G within the promoter of the proteinase‐3 gene (PRTN3) and the autoimmune disease Wegener's granulomatosis (WG). To further examine the strength of this association, we employed a family‐based design in which the inheritance of alternate alleles could be ascertained from the parents of affected and unaffected progeny. Genotype information for the study participants was derived from DNA samples from participants who collected buccal cells using a harvesting method that was non‐invasive and self‐administered. A brief questionnaire captured demographic data on the participants, the family relationships between participants, and the prevalence of autoimmune disease among family members. Samples were obtained on 132 individuals representing 43 WG cases and 89 unaffected controls. Thirty‐four nuclear families containing at least one unaffected sibling or parent of a WG case were represented in this sample. We found no evidence for an association between A‐564G and the likelihood of a WG diagnosis. We examined five additional SNPs and a sixth SNP haplotype within the PRTN3 promoter region in a family‐based association analysis and found no evidence that mutations within PRTN3 are associated with WG diagnosis.</description><subject>Autoimmune Diseases - epidemiology</subject><subject>Case-Control Studies</subject><subject>Demography</subject><subject>Female</subject><subject>Gene Frequency - genetics</subject><subject>Genetic Markers - genetics</subject><subject>Genetic Predisposition to Disease - genetics</subject><subject>Granulomatosis with Polyangiitis - diagnosis</subject><subject>Granulomatosis with Polyangiitis - genetics</subject><subject>Haplotypes - genetics</subject><subject>Humans</subject><subject>Male</subject><subject>Myeloblastin</subject><subject>Polymorphism, Single Nucleotide - genetics</subject><subject>Prevalence</subject><subject>Promoter Regions, Genetic - genetics</subject><subject>Serine Endopeptidases - genetics</subject><subject>Surveys and Questionnaires</subject><issn>1744-3121</issn><issn>1744-313X</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2005</creationdate><recordtype>article</recordtype><recordid>eNqNkV1PwjAUhhujEUX_gtmVXm32rB_rEm8IKGIIJgYDd003OjIcG7Yswr-3cwQvtUnT0_R9TtOnCHmAA3DjfhVARKlPgMyDEGMWuAlxsDtBF8eD02MdQgddWrvCmHBK8TnqAMchZzFcINorVbG3ufWqzFNekldrZT608bLKeDO91KU2d9ZbGlXWhTvbVi57hc4yVVh9fVi76P3pcdp_9sevw1G_N_ZTSljsx0DjkAihVRhxKmIMhPJEaJGKNFRRyhcASbNnC2BcMQGREgxjBWGiUod20W3bd2Oqz1rbrVznNtVFoUpd1VZygRklhP0ZhIhFnBPhgqINpqay1uhMbkzuXryXgGWjVq5kY002BmWjVv6olTuH3hzuqJO1XvyCB5cu8NAGvvJC7__dWI5eRq5wuN_iud3q3RF3vyF5RCImZ5OhZJPBdIDfqJyTbz6NlG0</recordid><startdate>200508</startdate><enddate>200508</enddate><creator>Cooley, P.</creator><creator>Taylor, K. 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To further examine the strength of this association, we employed a family‐based design in which the inheritance of alternate alleles could be ascertained from the parents of affected and unaffected progeny. Genotype information for the study participants was derived from DNA samples from participants who collected buccal cells using a harvesting method that was non‐invasive and self‐administered. A brief questionnaire captured demographic data on the participants, the family relationships between participants, and the prevalence of autoimmune disease among family members. Samples were obtained on 132 individuals representing 43 WG cases and 89 unaffected controls. Thirty‐four nuclear families containing at least one unaffected sibling or parent of a WG case were represented in this sample. We found no evidence for an association between A‐564G and the likelihood of a WG diagnosis. 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subjects	Autoimmune Diseases - epidemiology Case-Control Studies Demography Female Gene Frequency - genetics Genetic Markers - genetics Genetic Predisposition to Disease - genetics Granulomatosis with Polyangiitis - diagnosis Granulomatosis with Polyangiitis - genetics Haplotypes - genetics Humans Male Myeloblastin Polymorphism, Single Nucleotide - genetics Prevalence Promoter Regions, Genetic - genetics Serine Endopeptidases - genetics Surveys and Questionnaires
title	Analysis of a biomarker for Wegener's granulomatosis
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