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Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine

BACKGROUND: Single nucleotide polymorphisms (SNPs) are the most abundant source of genetic variation among individuals of a species. New genotyping technologies allow examining hundreds to thousands of SNPs in a single reaction for a wide range of applications such as genetic diversity analysis, lin...

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Autores principales: Chancerel, Emilie, Lepoittevin, Camille, Le Provost, Grégoire, Lin, Yao-Cheng, Jaramillo-Correa, Juan Pablo, Eckert, Andrew J, Wegrzyn, Jill L, Zelenika, Diana, Boland, Anne, Frigerio, Jean-Marc, Chaumeil, Philippe, Garnier-Géré, Pauline, Boury, Christophe, Grivet, Delphine, González-Martínez, Santiago C, Rouzé, Pierre, Van de Peer, Yves, Neale, David B, Cervera, Maria T, Kremer, Antoine, Plomion, Christophe
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3146957/
https://www.ncbi.nlm.nih.gov/pubmed/21767361
http://dx.doi.org/10.1186/1471-2164-12-368
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author Chancerel, Emilie
Lepoittevin, Camille
Le Provost, Grégoire
Lin, Yao-Cheng
Jaramillo-Correa, Juan Pablo
Eckert, Andrew J
Wegrzyn, Jill L
Zelenika, Diana
Boland, Anne
Frigerio, Jean-Marc
Chaumeil, Philippe
Garnier-Géré, Pauline
Boury, Christophe
Grivet, Delphine
González-Martínez, Santiago C
Rouzé, Pierre
Van de Peer, Yves
Neale, David B
Cervera, Maria T
Kremer, Antoine
Plomion, Christophe
author_facet Chancerel, Emilie
Lepoittevin, Camille
Le Provost, Grégoire
Lin, Yao-Cheng
Jaramillo-Correa, Juan Pablo
Eckert, Andrew J
Wegrzyn, Jill L
Zelenika, Diana
Boland, Anne
Frigerio, Jean-Marc
Chaumeil, Philippe
Garnier-Géré, Pauline
Boury, Christophe
Grivet, Delphine
González-Martínez, Santiago C
Rouzé, Pierre
Van de Peer, Yves
Neale, David B
Cervera, Maria T
Kremer, Antoine
Plomion, Christophe
author_sort Chancerel, Emilie
collection PubMed
description BACKGROUND: Single nucleotide polymorphisms (SNPs) are the most abundant source of genetic variation among individuals of a species. New genotyping technologies allow examining hundreds to thousands of SNPs in a single reaction for a wide range of applications such as genetic diversity analysis, linkage mapping, fine QTL mapping, association studies, marker-assisted or genome-wide selection. In this paper, we evaluated the potential of highly-multiplexed SNP genotyping for genetic mapping in maritime pine (Pinus pinaster Ait.), the main conifer used for commercial plantation in southwestern Europe. RESULTS: We designed a custom GoldenGate assay for 1,536 SNPs detected through the resequencing of gene fragments (707 in vitro SNPs/Indels) and from Sanger-derived Expressed Sequenced Tags assembled into a unigene set (829 in silico SNPs/Indels). Offspring from three-generation outbred (G2) and inbred (F2) pedigrees were genotyped. The success rate of the assay was 63.6% and 74.8% for in silico and in vitro SNPs, respectively. A genotyping error rate of 0.4% was further estimated from segregating data of SNPs belonging to the same gene. Overall, 394 SNPs were available for mapping. A total of 287 SNPs were integrated with previously mapped markers in the G2 parental maps, while 179 SNPs were localized on the map generated from the analysis of the F2 progeny. Based on 98 markers segregating in both pedigrees, we were able to generate a consensus map comprising 357 SNPs from 292 different loci. Finally, the analysis of sequence homology between mapped markers and their orthologs in a Pinus taeda linkage map, made it possible to align the 12 linkage groups of both species. CONCLUSIONS: Our results show that the GoldenGate assay can be used successfully for high-throughput SNP genotyping in maritime pine, a conifer species that has a genome seven times the size of the human genome. This SNP-array will be extended thanks to recent sequencing effort using new generation sequencing technologies and will include SNPs from comparative orthologous sequences that were identified in the present study, providing a wider collection of anchor points for comparative genomics among the conifers.
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spelling pubmed-31469572011-07-31 Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine Chancerel, Emilie Lepoittevin, Camille Le Provost, Grégoire Lin, Yao-Cheng Jaramillo-Correa, Juan Pablo Eckert, Andrew J Wegrzyn, Jill L Zelenika, Diana Boland, Anne Frigerio, Jean-Marc Chaumeil, Philippe Garnier-Géré, Pauline Boury, Christophe Grivet, Delphine González-Martínez, Santiago C Rouzé, Pierre Van de Peer, Yves Neale, David B Cervera, Maria T Kremer, Antoine Plomion, Christophe BMC Genomics Research Article BACKGROUND: Single nucleotide polymorphisms (SNPs) are the most abundant source of genetic variation among individuals of a species. New genotyping technologies allow examining hundreds to thousands of SNPs in a single reaction for a wide range of applications such as genetic diversity analysis, linkage mapping, fine QTL mapping, association studies, marker-assisted or genome-wide selection. In this paper, we evaluated the potential of highly-multiplexed SNP genotyping for genetic mapping in maritime pine (Pinus pinaster Ait.), the main conifer used for commercial plantation in southwestern Europe. RESULTS: We designed a custom GoldenGate assay for 1,536 SNPs detected through the resequencing of gene fragments (707 in vitro SNPs/Indels) and from Sanger-derived Expressed Sequenced Tags assembled into a unigene set (829 in silico SNPs/Indels). Offspring from three-generation outbred (G2) and inbred (F2) pedigrees were genotyped. The success rate of the assay was 63.6% and 74.8% for in silico and in vitro SNPs, respectively. A genotyping error rate of 0.4% was further estimated from segregating data of SNPs belonging to the same gene. Overall, 394 SNPs were available for mapping. A total of 287 SNPs were integrated with previously mapped markers in the G2 parental maps, while 179 SNPs were localized on the map generated from the analysis of the F2 progeny. Based on 98 markers segregating in both pedigrees, we were able to generate a consensus map comprising 357 SNPs from 292 different loci. Finally, the analysis of sequence homology between mapped markers and their orthologs in a Pinus taeda linkage map, made it possible to align the 12 linkage groups of both species. CONCLUSIONS: Our results show that the GoldenGate assay can be used successfully for high-throughput SNP genotyping in maritime pine, a conifer species that has a genome seven times the size of the human genome. This SNP-array will be extended thanks to recent sequencing effort using new generation sequencing technologies and will include SNPs from comparative orthologous sequences that were identified in the present study, providing a wider collection of anchor points for comparative genomics among the conifers. BioMed Central 2011-07-18 /pmc/articles/PMC3146957/ /pubmed/21767361 http://dx.doi.org/10.1186/1471-2164-12-368 Text en Copyright ©2011 Chancerel et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Chancerel, Emilie
Lepoittevin, Camille
Le Provost, Grégoire
Lin, Yao-Cheng
Jaramillo-Correa, Juan Pablo
Eckert, Andrew J
Wegrzyn, Jill L
Zelenika, Diana
Boland, Anne
Frigerio, Jean-Marc
Chaumeil, Philippe
Garnier-Géré, Pauline
Boury, Christophe
Grivet, Delphine
González-Martínez, Santiago C
Rouzé, Pierre
Van de Peer, Yves
Neale, David B
Cervera, Maria T
Kremer, Antoine
Plomion, Christophe
Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title_full Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title_fullStr Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title_full_unstemmed Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title_short Development and implementation of a highly-multiplexed SNP array for genetic mapping in maritime pine and comparative mapping with loblolly pine
title_sort development and implementation of a highly-multiplexed snp array for genetic mapping in maritime pine and comparative mapping with loblolly pine
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3146957/
https://www.ncbi.nlm.nih.gov/pubmed/21767361
http://dx.doi.org/10.1186/1471-2164-12-368
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