Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))

β-Thalassemia is a genetic disease caused by a defect in the production of the β-like globin chain. More than 200 known different variants can lead to the disease and are mainly found in populations that have been exposed to malaria parasites. We recently described a duplication of four nucleotides...

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Autores principales: Marchi, Nina, Pissard, Serge, Cliquennois, Manuel, Vasseur, Christian, Le Metayer, Nathalie, Mereau, Claude, Jouet, Jean Pierre, Georgel, Anne-France, Genin, Emmanuelle, Rose, Christian
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2015
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4538212/
https://www.ncbi.nlm.nih.gov/pubmed/25469539
http://dx.doi.org/10.1038/ejhg.2014.263
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author Marchi, Nina
Pissard, Serge
Cliquennois, Manuel
Vasseur, Christian
Le Metayer, Nathalie
Mereau, Claude
Jouet, Jean Pierre
Georgel, Anne-France
Genin, Emmanuelle
Rose, Christian
author_facet Marchi, Nina
Pissard, Serge
Cliquennois, Manuel
Vasseur, Christian
Le Metayer, Nathalie
Mereau, Claude
Jouet, Jean Pierre
Georgel, Anne-France
Genin, Emmanuelle
Rose, Christian
author_sort Marchi, Nina
collection PubMed
description β-Thalassemia is a genetic disease caused by a defect in the production of the β-like globin chain. More than 200 known different variants can lead to the disease and are mainly found in populations that have been exposed to malaria parasites. We recently described a duplication of four nucleotides in the first exon of β-globin gene in several families of patients living in Nord-Pas-de-Calais (France). Using the genotypes at 12 microsatellite markers surrounding the β-globin gene of four unrelated variant carriers plus an additional one recently discovered, we found that they shared a common haplotype indicating a founder effect that was estimated to have taken place 225 years ago (nine generations). In order to determine whether this variant arose in this region of Northern Europe or was introduced by migrants from regions of the world where thalassemia is endemic, we genotyped the first 4 unrelated variant carriers and 32 controls from Nord-Pas-de-Calais for 97 European ancestry informative markers (EAIMs). Using these EAIMs and comparing with population reference panels, we demonstrated that the variant carriers were very similar to the controls and were closer to North European populations than to South European or Middle-East populations. Rare β-thalassemia variants have already been described in patients sampled in non-endemic regions, but it is the first proof of a founder effect in Northern Europe.
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spelling pubmed-45382122015-08-21 Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA)) Marchi, Nina Pissard, Serge Cliquennois, Manuel Vasseur, Christian Le Metayer, Nathalie Mereau, Claude Jouet, Jean Pierre Georgel, Anne-France Genin, Emmanuelle Rose, Christian Eur J Hum Genet Article β-Thalassemia is a genetic disease caused by a defect in the production of the β-like globin chain. More than 200 known different variants can lead to the disease and are mainly found in populations that have been exposed to malaria parasites. We recently described a duplication of four nucleotides in the first exon of β-globin gene in several families of patients living in Nord-Pas-de-Calais (France). Using the genotypes at 12 microsatellite markers surrounding the β-globin gene of four unrelated variant carriers plus an additional one recently discovered, we found that they shared a common haplotype indicating a founder effect that was estimated to have taken place 225 years ago (nine generations). In order to determine whether this variant arose in this region of Northern Europe or was introduced by migrants from regions of the world where thalassemia is endemic, we genotyped the first 4 unrelated variant carriers and 32 controls from Nord-Pas-de-Calais for 97 European ancestry informative markers (EAIMs). Using these EAIMs and comparing with population reference panels, we demonstrated that the variant carriers were very similar to the controls and were closer to North European populations than to South European or Middle-East populations. Rare β-thalassemia variants have already been described in patients sampled in non-endemic regions, but it is the first proof of a founder effect in Northern Europe. Nature Publishing Group 2015-09 2014-12-03 /pmc/articles/PMC4538212/ /pubmed/25469539 http://dx.doi.org/10.1038/ejhg.2014.263 Text en Copyright © 2015 Macmillan Publishers Limited
spellingShingle Article
Marchi, Nina
Pissard, Serge
Cliquennois, Manuel
Vasseur, Christian
Le Metayer, Nathalie
Mereau, Claude
Jouet, Jean Pierre
Georgel, Anne-France
Genin, Emmanuelle
Rose, Christian
Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title_full Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title_fullStr Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title_full_unstemmed Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title_short Confirmation of a founder effect in a Northern European population of a new β-globin variant: HBB:c.23_26dup (codons 8/9 (+AGAA))
title_sort confirmation of a founder effect in a northern european population of a new β-globin variant: hbb:c.23_26dup (codons 8/9 (+agaa))
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4538212/
https://www.ncbi.nlm.nih.gov/pubmed/25469539
http://dx.doi.org/10.1038/ejhg.2014.263
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