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Dive into the research topics where Emmanuelle Bourneuf is active.

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Featured researches published by Emmanuelle Bourneuf.


Animal Genetics | 2011

Transcription specificity of the class Ib genes SLA-6, SLA-7 and SLA-8 of the swine major histocompatibility complex and comparison with class Ia genes.

S. Kusza; Laurence Flori; Yu Gao; Angélique Teillaud; Rui Hu; Gaetan Lemonnier; Z. Bosze; Emmanuelle Bourneuf; Silvia Vincent-Naulleau; Claire Rogel-Gaillard

Our aim was to analyse the transcription levels of the three non-classical class Ib genes SLA-6, SLA-7 and SLA-8 of the swine major histocompatibility complex in various tissues and conditions and to compare them to the transcription levels of classical class Ia genes. Twenty-five adult tissues from two pig breeds, pig renal PK15 cells infected with the Pseudorabies virus, and peripheral blood mononuclear cells (PBMCs) stimulated by lipopolysaccharide or a mixture of phorbol myristate acetate and ionomycin were included in our study. Relative transcription was quantified by quantitative real-time PCR. On average, in adult tissues and PBMCs and compared to SLA-6, the transcription level of SLA-Ia genes was 100-1000 times higher, the level of SLA-8 was 10-20 times higher, and that of SLA-7 was five times higher. Thus, SLA-8 is the most transcribed SLA-Ib gene, followed by the SLA-7 and SLA-6 genes. The highest transcription levels of SLA-Ib transcripts were found in the lymphoid organs, followed by the lung and the digestive tract. The tissue variability of expression levels was widest for the SLA-6 gene, with a 1:32 ratio between the lowest and highest levels in contrast to a 1:12 ratio for the SLA-7 and SLA-8 genes and a 1:16 ratio for the SLA-Ia genes. During PK-15 infection and PBMC stimulation, SLA-Ia and SLA-8 genes were downregulated, whereas SLA-6 and SLA-7 were upregulated, downregulated or not significantly modified. Our overall results confirm the tissue-wide transcription of the three SLA-Ib genes and suggest that they have complementary roles.


BMC Proceedings | 2011

Transcription variants of SLA-7, a swine non classical MHC class I gene

Rui Hu; Gaetan Lemonnier; Emmanuelle Bourneuf; Silvia Vincent-Naulleau; Claire Rogel-Gaillard

In pig, very little information is available on the non classical class I (Ib) genes of the Major Histocompatibility Complex (MHC) i.e. SLA-6, -7 and -8. Our aim was to focus on the transcription pattern of the SLA-7 gene. RT-PCR experiments were carried out with SLA-7 specific primers targeting either the full coding sequence (CDS) from exon 1 to the 3 prime untranslated region (3UTR) or a partial CDS from exon 4 to the 3UTR. We show that the SLA-7 gene expresses a full length transcript not yet identified that refines annotation of the gene with eight exons instead of seven as initially described from the existing RefSeq RNA. These two RNAs encode molecules that differ in cytoplasmic tail length. In this study, another SLA-7 transcript variant was characterized, which encodes a protein with a shorter alpha 3 domain, as a consequence of a splicing site within exon 4. Surprisingly, a cryptic non canonical GA-AG splicing site is used to generate this transcript variant. An additional SLA-7 variant was also identified in the 3UTR with a splicing site occurring 31 nucleotides downstream to the stop codon. In conclusion, the pig SLA-7 MHC class Ib gene presents a complex transcription pattern with two transcripts encoding various molecules and transcripts that do not alter the CDS and may be subject to post-transcriptional regulation.


Animal Genetics | 2014

KIT and melanoma predisposition in pigs: sequence variants and association analysis

A. Fernández-Rodríguez; Jordi Estellé; A. Blin; M. Muñoz; Francoise Créchet; Florence Demenais; Silvia Vincent-Naulleau; Emmanuelle Bourneuf

KIT mutations have been detected in different cancer subtypes, including melanoma. The gene also has been extensively studied in farm animals for its prominent role in coat color. The present work aimed at detecting KIT variants in a porcine model of cutaneous melanoma, the melanoblastoma-bearing Libechov Minipig (MeLiM). By sequencing exons and intron borders, 36 SNPs and one indel were identified. Of 10 coding SNPs, three were non-synonymous mutations, likely to affect the protein conformation. A promising variant, located in exon 19 (p.Val870Ala), was genotyped in a MeLiM × Duroc cross, and an association analysis was conducted on several melanoma-related traits. This variant showed a significant association with melanoma development, tumor ulceration and cutaneous invasion. In conclusion, although the KIT gene would not be a major causal gene for melanoma development in pig, its genetic variation could be influencing this trait.


Mammalian Genome | 2011

Genetic and functional evaluation of MITF as a candidate gene for cutaneous melanoma predisposition in pigs

Emmanuelle Bourneuf; Zhi-Qiang Du; Jordi Estellé; Hélène Gilbert; Francoise Créchet; Guillaume Piton; Denis Milan; Claudine Geffrotin; Mark Lathrop; Florence Demenais; Claire Rogel-Gaillard; Silvia Vincent-Naulleau

Cutaneous melanoma arises from transformed melanocytes and is caused mainly by environmental effects such as ultraviolet radiation and to a lesser extent by predisposing genetic variants. Only a few susceptibility genes for cutaneous melanoma have been identified so far in human; therefore, animal models represent a valuable alternative for genetic studies of this disease. In a previous quantitative trait locus (QTL) study, several susceptibility regions were identified in a swine biomedical model, the MeLiM (Melanoblastoma-bearing Libechov minipig) pigs. This article details the fine-mapping of a QTL located on SSC13 (Sus scrofa chromosome 13) through an increase in marker density. New microsatellites were used to confirm the results of the first analysis, and MITF (microphthalmia-associated transcription factor) was selected as a candidate gene for melanoma development. A single-marker association analysis was performed with single-nucleotide polymorphisms (SNPs) spread over the locus, but it did not reveal a significant association with diverse melanoma-related traits. In parallel, MITF alternative transcripts were characterized and their expression was investigated in different porcine tissues. The obtained results showed a complex transcriptional regulation concordant with the one present in other mammals. Notably, the ratio between MITF+ and MITF− isoforms in melanoma samples followed the same pattern as in human tumors, which highlights the adequacy of the MeLiM pig as a model for human melanoma. In conclusion, although MITF does not seem to be the causal gene of the QTL initially observed, we do not exclude a prominent role of its transcription and function in the outbreak and evolution of the tumors observed in pigs.


10th World Congress on Genetics Applied to Livestock Production | 2014

Rapid discovery of mutations responsible for sporadic dominant genetic defects in livestock using genome sequence data: enhancing the value of farm animals as model species

Aurélien Capitan; Pauline Michot; François Guillaume; Cécile Grohs; Anis Djari; S. Fritz; Sarah Barbey; Pauline Otz; Emmanuelle Bourneuf; Diane Esquerre; Yves Gallard; Christophe Klopp; Didier Boichard


Pigment Cell & Melanoma Research | 2014

Analysis of melanoma-related microRNAs expression during the spontaneous regression of cutaneous melanomas in MeLiM pigs.

Michael Baco; Chia-ying Chu; Stephan Bouet; Claire Rogel-Gaillard; Emmanuelle Bourneuf; Fabienne Le Provost; Chia-Yu Chu; Silvia Vincent-Naulleau


International Symposium of Microgenomics | 2014

Laser capture microdissection of skin melanocytes for the transcriptome characterization of a melanoma predisposition swine model

Jordi Estelle Fabrellas; Emmanuelle Bourneuf; Guillaume Piton; Jean Jacques Leplat; Stephan Bouet; Francoise Créchet; Patrice Martin; Claudia Bevilacqua; Silvia Vincent-Naulleau


33rd Conference of the International Society of Animal Genetics (ISAG) | 2012

Whole genome re-sequencing of the MeLiM porcine model for cutaneous melanoma

Jordi Estellé; Diane Esquerre; Olivier Bouchez; Silvia Vincent-Naulleau; Per Wahlberg; Emmanuelle Bourneuf


18. Meeting of the European Society for Pigment Cell Research (ESPCR – 2013) | 2012

A large animal model for human Tietz syndrome: In vivo insights into MITF R217del mutation

Emmanuelle Bourneuf; Aurélien Capitan; Francoise Créchet; Stephan Bouet; S. Fritz; Diane Esquerre; Sarah Barbey; Didier Boichard; Dominique Rocha; Patrick Costiou


IPCC 2011 - XXIst International Pigment Cell Conference | 2011

Detection of CNVs throughout the genome of a porcine melanoma model.

Jordi Corominas; Jordi Estellé; Yuliaxis Ramayo-Caldas; Mark Lathrop; Florence Demenais; Claire Rogel-Gaillard; Silvia Vincent-Naulleau; Josep-Maria Folch; Emmanuelle Bourneuf

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Silvia Vincent-Naulleau

Institut national de la recherche agronomique

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Claire Rogel-Gaillard

Institut national de la recherche agronomique

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Francoise Créchet

Institut national de la recherche agronomique

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Guillaume Piton

Institut national de la recherche agronomique

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Stephan Bouet

Institut national de la recherche agronomique

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Jordi Estellé

Université Paris-Saclay

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Diane Esquerre

Institut national de la recherche agronomique

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Denis Milan

Institut national de la recherche agronomique

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Aurélien Capitan

Institut national de la recherche agronomique

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