Literature DB >> 20107036

Early transcription from the maternal genome controlling blastomere integrity in mouse two-cell-stage embryos.

Zhiming Han1, Namdori R Mtango, Zhisheng Zhong, Rita Vassena, Keith E Latham.   

Abstract

Blastomere cytofragmentation in mammalian embryos poses a significant problem in applied and clinical embryology. Mouse two-cell-stage embryos display strain-dependent differences in the rate of cytofragmentation, with a high rate observed in C3H/HeJ embryos and a lower rate observed in C57BL/6 embryos. The maternally inherited genome exerts the strongest effect on the process, with lesser effects mediated by the paternally inherited genome and the ooplasm. The effect of the maternal genome is transcription dependent and independent of the mitochondrial strain of origin. To identify molecular mechanisms that underlie cytofragmentation, we evaluated transcriptional activities of embryos possessing maternal pronuclei (mPN) of different origins. The mPN from C57BL/6 and C3H/HeJ strains directed specific transcription at the two-cell stage of mRNAs corresponding to 935 and 864 Affymetrix probe set IDs, respectively. Comparing transcriptomes of two-cell-stage embryos with different mPN revealed 64 transcribed genes with differential expression (1.4-fold or greater). Some of these genes occupy molecular pathways that may regulate cytofragmentation via a combination of effects related to apoptosis and effects on the cytoskeleton. These results implicate specific molecular mechanisms that may regulate cytofragmentation in early mammalian embryos. The most striking effect of mPN strain of origin on gene expression was on adenylate cyclase 2 (Adcy2). Treatment with dibutyryl cAMP (dbcAMP) elicits a high rate and severe form of cytofragmentation, and the effective dbcAMP concentration varies with maternal genotype. An activator of exchange proteins directly activated by cAMP (EPACs, or RAPGEF 3 and 4) 8-pCPT-2'-O-methyl-cAMP, elicits a high level of fragmentation while the PKA-specific activator N6-benzoyl-cAMP does not. Inhibition of A kinase anchor protein activities with st-Ht31 induces fragmentation. Inhibition of phosphatidylinositol 3-kinase signaling also induces fragmentation. These results reveal novel mechanisms by which maternal genotype affects cytofragmentation, including a system of opposing signaling pathways that most likely operate by controlling cytoskeletal function.

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Year:  2010        PMID: 20107036      PMCID: PMC2867389          DOI: 10.1152/ajpcell.00393.2009

Source DB:  PubMed          Journal:  Am J Physiol Cell Physiol        ISSN: 0363-6143            Impact factor:   4.249


  61 in total

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8.  Analysis of litter size and weight in mice differing in Ped gene phenotype and the Q region of the H-2 complex.

Authors:  C M Warner; M S Brownell; M F Rothschild
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9.  Dose-response effects of glucose, insulin, and glucagon on mouse pre-embryo development.

Authors:  M P Diamond; Z Y Pettway; J Logan; K Moley; W Vaughn; A H DeCherney
Journal:  Metabolism       Date:  1991-06       Impact factor: 8.694

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Authors:  C M Warner; P Panda; C D Almquist; Y Xu
Journal:  J Reprod Fertil       Date:  1993-09
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  4 in total

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Authors:  Nicola A Martino; Maria E Dell'aquila; Rosa A Cardone; Bence Somoskoi; Giovanni M Lacalandra; Sandor Cseh
Journal:  Reprod Biol Endocrinol       Date:  2013-04-03       Impact factor: 5.211

Review 4.  Gasotransmitters in Gametogenesis and Early Development: Holy Trinity for Assisted Reproductive Technology-A Review.

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Journal:  Oxid Med Cell Longev       Date:  2016-08-08       Impact factor: 6.543

  4 in total

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