Dissection of Genetic Factors Modulating Fetal Growth in Cattle Indicates a Substantial Role of the Non-SMC Condensin I Complex, Subunit G (NCAPG) Gene

Author:

Eberlein Annett1,Takasuga Akiko2,Setoguchi Kouji3,Pfuhl Ralf4,Flisikowski Krzysztof5,Fries Ruedi5,Klopp Norman6,Fürbass Rainer1,Weikard Rosemarie1,Kühn Christa1

Affiliation:

1. Research Unit Molecular Biology and

2. Shirikawa Institute of Animal Genetics, Japan Livestock Technology Association, Odakura, Nishigo, Fukushima 961-8062, Japan

3. Cattle Breeding Development Institute of Kagoshima Prefecture, Osumi, So, Kagoshima 899-8212, Japan

4. Research Unit Muscle Biology and Growth, Research Institute for the Biology of Farm Animals, 18196 Dummerstorf, Germany

5. Chair of Animal Breeding, Technische Universität München, 85350 Freising, Germany and

6. Institute of Epidemiology, Helmholtz Zentrum München, 85764 Neuherberg, Germany

Abstract

Abstract The increasing evidence of fetal developmental effects on postnatal life, the still unknown fetal growth mechanisms impairing offspring generated by somatic nuclear transfer techniques, and the impact on stillbirth and dystocia in conventional reproduction have generated increasing attention toward mammalian fetal growth. We identified a highly significant quantitative trait locus (QTL) affecting fetal growth on bovine chromosome 6 in a specific resource population, which was set up by consistent use of embryo transfer and foster mothers and, thus, enabled dissection of fetal-specific genetic components of fetal growth. Merging our data with results from other cattle populations differing in historical and geographical origin and with comparative data from human whole-genome association mapping suggests that a nonsynonymous polymorphism in the non-SMC condensin I complex, subunit G (NCAPG) gene, NCAPG c.1326T>G, is the potential cause of the identified QTL resulting in divergent bovine fetal growth. NCAPG gene expression data in fetal placentomes with different NCAPG c.1326T>G genotypes, which are in line with recent results about differential NCAPG expression in placentomes from studies on assisted reproduction techniques, indicate that the NCAPG locus may give valuable information on the specific mechanisms regulating fetal growth in mammals.

Publisher

Oxford University Press (OUP)

Subject

Genetics

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