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Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population

The high risk of metabolic disease traits in Polynesians may be partly explained by elevated prevalence of genetic variants involved in energy metabolism. The genetics of Polynesian populations has been shaped by island hoping migration events which have possibly favoured thrifty genes. The aim of t...

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Autores principales: Benton, Miles, Macartney-Coxson, Donia, Eccles, David, Griffiths, Lyn, Chambers, Geoff, Lea, Rod
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325929/
https://www.ncbi.nlm.nih.gov/pubmed/22514703
http://dx.doi.org/10.1371/journal.pone.0035026
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author Benton, Miles
Macartney-Coxson, Donia
Eccles, David
Griffiths, Lyn
Chambers, Geoff
Lea, Rod
author_facet Benton, Miles
Macartney-Coxson, Donia
Eccles, David
Griffiths, Lyn
Chambers, Geoff
Lea, Rod
author_sort Benton, Miles
collection PubMed
description The high risk of metabolic disease traits in Polynesians may be partly explained by elevated prevalence of genetic variants involved in energy metabolism. The genetics of Polynesian populations has been shaped by island hoping migration events which have possibly favoured thrifty genes. The aim of this study was to sequence the mitochondrial genome in a group of Maoris in an effort to characterise genome variation in this Polynesian population for use in future disease association studies. We sequenced the complete mitochondrial genomes of 20 non-admixed Maori subjects using Affymetrix technology. DNA diversity analyses showed the Maori group exhibited reduced mitochondrial genome diversity compared to other worldwide populations, which is consistent with historical bottleneck and founder effects. Global phylogenetic analysis positioned these Maori subjects specifically within mitochondrial haplogroup - B4a1a1. Interestingly, we identified several novel variants that collectively form new and unique Maori motifs – B4a1a1c, B4a1a1a3 and B4a1a1a5. Compared to ancestral populations we observed an increased frequency of non-synonymous coding variants of several mitochondrial genes in the Maori group, which may be a result of positive selection and/or genetic drift effects. In conclusion, this study reports the first complete mitochondrial genome sequence data for a Maori population. Overall, these new data reveal novel mitochondrial genome signatures in this Polynesian population and enhance the phylogenetic picture of maternal ancestry in Oceania. The increased frequency of several mitochondrial coding variants makes them good candidates for future studies aimed at assessment of metabolic disease risk in Polynesian populations.
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spelling pubmed-33259292012-04-18 Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population Benton, Miles Macartney-Coxson, Donia Eccles, David Griffiths, Lyn Chambers, Geoff Lea, Rod PLoS One Research Article The high risk of metabolic disease traits in Polynesians may be partly explained by elevated prevalence of genetic variants involved in energy metabolism. The genetics of Polynesian populations has been shaped by island hoping migration events which have possibly favoured thrifty genes. The aim of this study was to sequence the mitochondrial genome in a group of Maoris in an effort to characterise genome variation in this Polynesian population for use in future disease association studies. We sequenced the complete mitochondrial genomes of 20 non-admixed Maori subjects using Affymetrix technology. DNA diversity analyses showed the Maori group exhibited reduced mitochondrial genome diversity compared to other worldwide populations, which is consistent with historical bottleneck and founder effects. Global phylogenetic analysis positioned these Maori subjects specifically within mitochondrial haplogroup - B4a1a1. Interestingly, we identified several novel variants that collectively form new and unique Maori motifs – B4a1a1c, B4a1a1a3 and B4a1a1a5. Compared to ancestral populations we observed an increased frequency of non-synonymous coding variants of several mitochondrial genes in the Maori group, which may be a result of positive selection and/or genetic drift effects. In conclusion, this study reports the first complete mitochondrial genome sequence data for a Maori population. Overall, these new data reveal novel mitochondrial genome signatures in this Polynesian population and enhance the phylogenetic picture of maternal ancestry in Oceania. The increased frequency of several mitochondrial coding variants makes them good candidates for future studies aimed at assessment of metabolic disease risk in Polynesian populations. Public Library of Science 2012-04-13 /pmc/articles/PMC3325929/ /pubmed/22514703 http://dx.doi.org/10.1371/journal.pone.0035026 Text en Benton 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
Benton, Miles
Macartney-Coxson, Donia
Eccles, David
Griffiths, Lyn
Chambers, Geoff
Lea, Rod
Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title_full Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title_fullStr Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title_full_unstemmed Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title_short Complete Mitochondrial Genome Sequencing Reveals Novel Haplotypes in a Polynesian Population
title_sort complete mitochondrial genome sequencing reveals novel haplotypes in a polynesian population
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3325929/
https://www.ncbi.nlm.nih.gov/pubmed/22514703
http://dx.doi.org/10.1371/journal.pone.0035026
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