Mosaicism of Solid Gold Supports the Causality of a Noncoding A-to-G Transition in the Determinism of the Callipyge Phenotype

To identify the callipyge mutation, we have resequenced 184 kb spanning the DLK1-, GTL2-, PEG11-, and MEG8-imprinted domain and have identified an A-to-G transition in a highly conserved dodecamer motif between DLK1 and GTL2. This was the only difference found between the callipyge (CLPG) allele and...

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Veröffentlicht in:	Genetics (Austin) 2003-01, Vol.163 (1), p.453-456
Hauptverfasser:	Smit, Maria, Segers, Karin, Carrascosa, Laura Garcia, Shay, Tracy, Baraldi, Francesca, Gyapay, Gabor, Snowder, Gary, Georges, Michel, Cockett, Noelle, Charlier, Carole
Format:	Artikel
Sprache:	eng
Schlagworte:	Animals Base Sequence Causality Genetics Genetics & genetic processes Gold Génétique & processus génétiques Life sciences Molecular Sequence Data Mosaicism - genetics Muscular Diseases - genetics Médecine vétérinaire & santé animale Point Mutation Sciences du vivant Sheep - abnormalities Sheep - genetics Sheep/abnormalities/genetics Veterinary medicine & animal health
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Zusammenfassung:	To identify the callipyge mutation, we have resequenced 184 kb spanning the DLK1-, GTL2-, PEG11-, and MEG8-imprinted domain and have identified an A-to-G transition in a highly conserved dodecamer motif between DLK1 and GTL2. This was the only difference found between the callipyge (CLPG) allele and a phylogenetically closely related wild-type allele. We report that this SNP is in perfect association with the callipyge genotype. The demonstration that Solid Gold-the alleged founder ram of the callipyge flock-is mosaic for this SNP virtually proves the causality of this SNP in the determinism of the callipyge phenotype.
ISSN:	0016-6731 1943-2631 1943-2631
DOI:	10.1093/genetics/163.1.453