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Parallel Selection on TRPV6 in Human Populations

We identified and examined a candidate gene for local directional selection in Europeans, TRPV6, and conclude that selection has acted on standing genetic variation at this locus, creating parallel soft sweep events in humans. A novel modification of the extended haplotype homozygosity (EHH) test wa...

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Autores principales: Hughes, David A., Tang, Kun, Strotmann, Rainer, Schöneberg, Torsten, Prenen, Jean, Nilius, Bernd, Stoneking, Mark
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2008
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2246018/
https://www.ncbi.nlm.nih.gov/pubmed/18301763
http://dx.doi.org/10.1371/journal.pone.0001686
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author Hughes, David A.
Tang, Kun
Strotmann, Rainer
Schöneberg, Torsten
Prenen, Jean
Nilius, Bernd
Stoneking, Mark
author_facet Hughes, David A.
Tang, Kun
Strotmann, Rainer
Schöneberg, Torsten
Prenen, Jean
Nilius, Bernd
Stoneking, Mark
author_sort Hughes, David A.
collection PubMed
description We identified and examined a candidate gene for local directional selection in Europeans, TRPV6, and conclude that selection has acted on standing genetic variation at this locus, creating parallel soft sweep events in humans. A novel modification of the extended haplotype homozygosity (EHH) test was utilized, which compares EHH for a single allele across populations, to investigate the signature of selection at TRPV6 and neighboring linked loci in published data sets for Europeans, Asians and African-Americans, as well as in newly-obtained sequence data for additional populations. We find that all non-African populations carry a signature of selection on the same haplotype at the TRPV6 locus. The selective footprints, however, are significantly differentiated between non-African populations and estimated to be younger than an ancestral population of non-Africans. The possibility of a single selection event occurring in an ancestral population of non-Africans was tested by simulations and rejected. The putatively-selected TRPV6 haplotype contains three candidate sites for functional differences, namely derived non-synonymous substitutions C157R, M378V and M681T. Potential functional differences between the ancestral and derived TRPV6 proteins were investigated by cloning the ancestral and derived forms, transfecting cell lines, and carrying out electrophysiology experiments via patch clamp analysis. No statistically-significant differences in biophysical channel function were found, although one property of the protein, namely Ca(2+) dependent inactivation, may show functionally relevant differences between the ancestral and derived forms. Although the reason for selection on this locus remains elusive, this is the first demonstration of a widespread parallel selection event acting on standing genetic variation in humans, and highlights the utility of between population EHH statistics.
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spelling pubmed-22460182008-02-27 Parallel Selection on TRPV6 in Human Populations Hughes, David A. Tang, Kun Strotmann, Rainer Schöneberg, Torsten Prenen, Jean Nilius, Bernd Stoneking, Mark PLoS One Research Article We identified and examined a candidate gene for local directional selection in Europeans, TRPV6, and conclude that selection has acted on standing genetic variation at this locus, creating parallel soft sweep events in humans. A novel modification of the extended haplotype homozygosity (EHH) test was utilized, which compares EHH for a single allele across populations, to investigate the signature of selection at TRPV6 and neighboring linked loci in published data sets for Europeans, Asians and African-Americans, as well as in newly-obtained sequence data for additional populations. We find that all non-African populations carry a signature of selection on the same haplotype at the TRPV6 locus. The selective footprints, however, are significantly differentiated between non-African populations and estimated to be younger than an ancestral population of non-Africans. The possibility of a single selection event occurring in an ancestral population of non-Africans was tested by simulations and rejected. The putatively-selected TRPV6 haplotype contains three candidate sites for functional differences, namely derived non-synonymous substitutions C157R, M378V and M681T. Potential functional differences between the ancestral and derived TRPV6 proteins were investigated by cloning the ancestral and derived forms, transfecting cell lines, and carrying out electrophysiology experiments via patch clamp analysis. No statistically-significant differences in biophysical channel function were found, although one property of the protein, namely Ca(2+) dependent inactivation, may show functionally relevant differences between the ancestral and derived forms. Although the reason for selection on this locus remains elusive, this is the first demonstration of a widespread parallel selection event acting on standing genetic variation in humans, and highlights the utility of between population EHH statistics. Public Library of Science 2008-02-27 /pmc/articles/PMC2246018/ /pubmed/18301763 http://dx.doi.org/10.1371/journal.pone.0001686 Text en Hughes et al. http://creativecommons.org/licenses/by/4.0/ 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 author and source are properly credited.
spellingShingle Research Article
Hughes, David A.
Tang, Kun
Strotmann, Rainer
Schöneberg, Torsten
Prenen, Jean
Nilius, Bernd
Stoneking, Mark
Parallel Selection on TRPV6 in Human Populations
title Parallel Selection on TRPV6 in Human Populations
title_full Parallel Selection on TRPV6 in Human Populations
title_fullStr Parallel Selection on TRPV6 in Human Populations
title_full_unstemmed Parallel Selection on TRPV6 in Human Populations
title_short Parallel Selection on TRPV6 in Human Populations
title_sort parallel selection on trpv6 in human populations
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2246018/
https://www.ncbi.nlm.nih.gov/pubmed/18301763
http://dx.doi.org/10.1371/journal.pone.0001686
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