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1 April 2008 Identification of Genes Aberrantly Expressed in Mouse Embryonic Stem Cell-Cloned Blastocysts
Yuko Jincho, Yusuke Sotomaru, Manabu Kawahara, Yukiko Ono, Hidehiko Ogawa, Yayoi Obata, Tomohiro Kono
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Abstract

During development, cloned embryos often undergo embryonic arrest at any stage of embryogenesis, leading to diverse morphological abnormalities. The long-term effects resulting from embryo cloning procedures would manifest after birth as early death, obesity, various functional disorders, and so forth. Despite extensive studies, the parameters affecting the developmental features of cloned embryos remain unclear. The present study carried out extensive gene expression analysis to screen a cluster of genes aberrantly expressed in embryonic stem cell-cloned blastocysts. Differential screening of cDNA subtraction libraries revealed 224 differentially expressed genes in the cloned blastocysts: eighty-five were identified by the BLAST search as known genes performing a wide range of functions. To confirm their differential expression, quantitative gene expression analyses were performed by real-time PCR using single blastocysts. The genes Skp1a, Canx, Ctsd, Timd2, and Psmc6 were significantly up-regulated, whereas Aqp3, Ak3l1, Rhot1, Sf3b3, Nid1, mt-Rnr2, mt-Nd1, mt-Cytb, and mt-Co2 were significantly down-regulated in the majority of embryonic stem cell-cloned embryos. Our results suggest that an extraordinarily high frequency of multiple functional disorders caused by the aberrant expression of various genes in the blastocyst stage is involved in developmental arrest and various other disorders in cloned embryos.

Yuko Jincho, Yusuke Sotomaru, Manabu Kawahara, Yukiko Ono, Hidehiko Ogawa, Yayoi Obata, and Tomohiro Kono "Identification of Genes Aberrantly Expressed in Mouse Embryonic Stem Cell-Cloned Blastocysts," Biology of Reproduction 78(4), 568-576, (1 April 2008). https://doi.org/10.1095/biolreprod.107.064634
Received: 30 July 2007; Accepted: 1 October 2007; Published: 1 April 2008
KEYWORDS
cDNA subtraction
early development
embryo
ES cell clone
gene expression
gene regulation
nuclear transfer
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