IBC CARe microarray allelic population prevalences in an American Indian population.

IBC CARe microarray allelic population prevalences in an American Indian population.

The prevalence of variant alleles among single nucleotide polymorphisms (SNPs) is not well known for many minority populations. These population allele frequencies (PAFs) are necessary to guide genetic epidemiology studies and to understand the population specific contribution of these variants to d...

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Main Authors: Lyle G Best, Cindy M Anderson, Richa Saxena, Berta Almoguera, Hareesh Chandrupatla, Candelaria Martin, Gilbert Falcon, Kylie Keplin, Nichole Pearson, Brendan J Keating
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3765406?pdf=render
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spelling doaj-af2f2eb0c8494a75aa310d70148cc0ad2020-11-25T01:24:02ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0189e7508010.1371/journal.pone.0075080IBC CARe microarray allelic population prevalences in an American Indian population.Lyle G BestCindy M AndersonRicha SaxenaBerta AlmogueraHareesh ChandrupatlaCandelaria MartinGilbert FalconKylie KeplinNichole PearsonBrendan J KeatingThe prevalence of variant alleles among single nucleotide polymorphisms (SNPs) is not well known for many minority populations. These population allele frequencies (PAFs) are necessary to guide genetic epidemiology studies and to understand the population specific contribution of these variants to disease risk. Large differences in PAF among certain functional groups of genes could also indicate possible selection pressure or founder effects of interest. The 50K SNP, custom genotyping microarray (CARe) was developed, focusing on about 2,000 candidate genes and pathways with demonstrated pathophysiologic influence on cardiovascular disease (CVD).The CARe microarray was used to genotype 216 unaffected controls in a study of pre-eclampsia among a Northern Plains, American Indian tribe. The allelic prevalences of 34,240 SNPs suitable for analysis, were determined and compared with corresponding HapMap prevalences for the Caucasian population. Further analysis was conducted to compare the frequency of statistically different prevalences among functionally related SNPs, as determined by the DAVID Bioinformatics Resource.Of the SNPs with PAFs in both datasets, 9.8%,37.2% and 47.1% showed allele frequencies among the American Indian population greater than, less than and either greater or less than (respectively) the HapMap Caucasian population. The 2,547 genes were divided into 53 functional groups using the highest stringency criteria. While none of these groups reached the Bonferroni corrected p value of 0.00094, there were 7 of these 53 groups with significantly more or less differing PAFs, each with a probability of less than 0.05 and an overall probability of 0.0046.In comparison to the HapMap Caucasian population, there are substantial differences in the prevalence among an American Indian community of SNPs related to CVD. Certain functional groups of genes and related SNPs show possible evidence of selection pressure or founder effects.http://europepmc.org/articles/PMC3765406?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Lyle G Best
Cindy M Anderson
Richa Saxena
Berta Almoguera
Hareesh Chandrupatla
Candelaria Martin
Gilbert Falcon
Kylie Keplin
Nichole Pearson
Brendan J Keating
spellingShingle Lyle G Best
Cindy M Anderson
Richa Saxena
Berta Almoguera
Hareesh Chandrupatla
Candelaria Martin
Gilbert Falcon
Kylie Keplin
Nichole Pearson
Brendan J Keating
IBC CARe microarray allelic population prevalences in an American Indian population.
PLoS ONE
author_facet Lyle G Best
Cindy M Anderson
Richa Saxena
Berta Almoguera
Hareesh Chandrupatla
Candelaria Martin
Gilbert Falcon
Kylie Keplin
Nichole Pearson
Brendan J Keating
author_sort Lyle G Best
title IBC CARe microarray allelic population prevalences in an American Indian population.
title_short IBC CARe microarray allelic population prevalences in an American Indian population.
title_full IBC CARe microarray allelic population prevalences in an American Indian population.
title_fullStr IBC CARe microarray allelic population prevalences in an American Indian population.
title_full_unstemmed IBC CARe microarray allelic population prevalences in an American Indian population.
title_sort ibc care microarray allelic population prevalences in an american indian population.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description The prevalence of variant alleles among single nucleotide polymorphisms (SNPs) is not well known for many minority populations. These population allele frequencies (PAFs) are necessary to guide genetic epidemiology studies and to understand the population specific contribution of these variants to disease risk. Large differences in PAF among certain functional groups of genes could also indicate possible selection pressure or founder effects of interest. The 50K SNP, custom genotyping microarray (CARe) was developed, focusing on about 2,000 candidate genes and pathways with demonstrated pathophysiologic influence on cardiovascular disease (CVD).The CARe microarray was used to genotype 216 unaffected controls in a study of pre-eclampsia among a Northern Plains, American Indian tribe. The allelic prevalences of 34,240 SNPs suitable for analysis, were determined and compared with corresponding HapMap prevalences for the Caucasian population. Further analysis was conducted to compare the frequency of statistically different prevalences among functionally related SNPs, as determined by the DAVID Bioinformatics Resource.Of the SNPs with PAFs in both datasets, 9.8%,37.2% and 47.1% showed allele frequencies among the American Indian population greater than, less than and either greater or less than (respectively) the HapMap Caucasian population. The 2,547 genes were divided into 53 functional groups using the highest stringency criteria. While none of these groups reached the Bonferroni corrected p value of 0.00094, there were 7 of these 53 groups with significantly more or less differing PAFs, each with a probability of less than 0.05 and an overall probability of 0.0046.In comparison to the HapMap Caucasian population, there are substantial differences in the prevalence among an American Indian community of SNPs related to CVD. Certain functional groups of genes and related SNPs show possible evidence of selection pressure or founder effects.
url http://europepmc.org/articles/PMC3765406?pdf=render
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