Literature DB >> 23307892

Systems genetics implicates cytoskeletal genes in oocyte control of cloned embryo quality.

Yong Cheng1, John Gaughan, Uros Midic, Zhiming Han, Cheng-Guang Liang, Bela G Patel, Keith E Latham.   

Abstract

Cloning by somatic cell nuclear transfer is an important technology, but remains limited due to poor rates of success. Identifying genes supporting clone development would enhance our understanding of basic embryology, improve applications of the technology, support greater understanding of establishing pluripotent stem cells, and provide new insight into clinically important determinants of oocyte quality. For the first time, a systems genetics approach was taken to discover genes contributing to the ability of an oocyte to support early cloned embryo development. This identified a primary locus on mouse chromosome 17 and potential loci on chromosomes 1 and 4. A combination of oocyte transcriptome profiling data, expression correlation analysis, and functional and network analyses yielded a short list of likely candidate genes in two categories. The major category-including two genes with the strongest genetic associations with the traits (Epb4.1l3 and Dlgap1)-encodes proteins associated with the subcortical cytoskeleton and other cytoskeletal elements such as the spindle. The second category encodes chromatin and transcription regulators (Runx1t1, Smchd1, and Chd7). Smchd1 promotes X chromosome inactivation, whereas Chd7 regulates expression of pluripotency genes. Runx1t1 has not been associated with these processes, but acts as a transcriptional repressor. The finding that cytoskeleton-associated proteins may be key determinants of early clone development highlights potential roles for cytoplasmic components of the oocyte in supporting nuclear reprogramming. The transcriptional regulators identified may contribute to the overall process as downstream effectors.

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Year:  2013        PMID: 23307892      PMCID: PMC3584004          DOI: 10.1534/genetics.112.148866

Source DB:  PubMed          Journal:  Genetics        ISSN: 0016-6731            Impact factor:   4.562


  88 in total

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5.  Oocyte spindle proteomics analysis leading to rescue of chromosome congression defects in cloned embryos.

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2.  SMCHD1 terminates the first embryonic genome activation event in mouse two-cell embryos and contributes to a transcriptionally repressive state.

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4.  Novel key roles for structural maintenance of chromosome flexible domain containing 1 (Smchd1) during preimplantation mouse development.

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5.  Embryotropic actions of follistatin: paracrine and autocrine mediators of oocyte competence and embryo developmental progression.

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6.  Zinc supplementation during in vitro maturation increases the production efficiency of cloned pigs.

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