Abstract

The primary objective of oocyte development is to become an embryo, one capable of development to healthy offspring. Successful oocyte-to-embryo transition depends upon the completion of meiosis and the utilization of maternal factors stored during oocyte development. This ReproGenomics Program Project has produced three infertile mutants that are unable to complete this transition and, therefore, present excellent opportunities to discover novel mechanisms that control it. Meiotic arrest 1 (marf1) mutant oocytes are unable to undergo germinal vesicle breakdown (GVB) and are ovulated at the immature (GV) stage. Oocyte maturation defective (omd1) and bromodomain and WD repeat domain containing 1 (Brwd1) mutant eggs cannot develop beyond the 2 pronuclear stage after insemination. The marf1 and omd1 mutations affect only females, while the Brwd1 mutation affects both males and females.
Aim 1 is to discover new pathways regulating the GV-to-GVB transition. The gene harboring the marf1 mutation does not encode a component of maturation promoting factor (MPF), or any of its known proximal regulators. Hypotheses that MARF1 protein is either a previously unknown regulator of MPF activity or a key oocyte-specific component of pathways regulated by MPF will be tested.
In Aim 2, ovulated GV-arrested marf1 mutant oocytes, and oocyte culture systems, will be used to test the hypothesis that some aspects of cytoplasmic maturation, particularly the degradation of specific groups of transcripts during the GV-to-MII transition, and processes that prepare for egg activation, occur independently of nuclear maturation.
Aim 3 is to discover new pathways regulating the oocyte-to-embryo transition using the Brwd1 and omd1 mutations, and a knockout of the oocyte-specific gene zygotic arrest 1 (Zar1) gene. The hypothesis that BRWD1, ZAR1, and OMD1 proteins are fundamental determinants of oocyte quality and that mutant alleles of genes encoding them disrupt key pathways needed to transit from GV-stage oocyte to preimplantation embryo will be tested.

Public Health Relevance

By discovering novel mechanisms controlling the oocyte-to-embryo transition, this work will provide insight into common human female infertility syndromes. The studies proposed here will discover molecules, pathways, and processes needed to produce good eggs capable of maturation and undergoing early embryogenesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD042137-08
Application #
8120790
Study Section
Special Emphasis Panel (ZHD1)
Project Start
Project End
Budget Start
2010-07-01
Budget End
2011-06-30
Support Year
8
Fiscal Year
2010
Total Cost
$165,346
Indirect Cost

  Institution

Name
Jackson Laboratory
Department
Type
DUNS #
042140483
City
Bar Harbor
State
ME
Country
United States
Zip Code
04609

  Publications

Hays, E; Majchrzak, N; Daniel, V et al. (2017) Spermatogenesis associated 22 is required for DNA repair and synapsis of homologous chromosomes in mouse germ cells. Andrology 5:299-312
Fujiwara, Yasuhiro; Matsumoto, Hirokazu; Akiyama, Kouyou et al. (2015) An ENU-induced mutation in the mouse Rnf212 gene is associated with male meiotic failure and infertility. Reproduction 149:67-74
Sun, Fengyun; Fujiwara, Yasuhiro; Reinholdt, Laura G et al. (2015) Nuclear localization of PRDM9 and its role in meiotic chromatin modifications and homologous synapsis. Chromosoma 124:397-415
Pattabiraman, Shrivatsav; Baumann, Claudia; Guisado, Daniela et al. (2015) Mouse BRWD1 is critical for spermatid postmeiotic transcription and female meiotic chromosome stability. J Cell Biol 208:53-69
Harris, Tanya P; Schimenti, Kerry J; Munroe, Robert J et al. (2014) IQ motif-containing G (Iqcg) is required for mouse spermiogenesis. G3 (Bethesda) 4:367-72
Schimenti, Kerry J; Feuer, Sky K; Griffin, Laurie B et al. (2013) AKAP9 is essential for spermatogenesis and sertoli cell maturation in mice. Genetics 194:447-57
Gómez, Rocío; Jordan, Philip W; Viera, Alberto et al. (2013) Dynamic localization of SMC5/6 complex proteins during mammalian meiosis and mitosis suggests functions in distinct chromosome processes. J Cell Sci 126:4239-52
Bentson, L F; Agbor, V A; Agbor, L N et al. (2013) New point mutation in Golga3 causes multiple defects in spermatogenesis. Andrology 1:440-50
Luo, Mengcheng; Yang, Fang; Leu, N Adrian et al. (2013) MEIOB exhibits single-stranded DNA-binding and exonuclease activities and is essential for meiotic recombination. Nat Commun 4:2788
Li, Xin Zhiguo; Roy, Christian K; Dong, Xianjun et al. (2013) An ancient transcription factor initiates the burst of piRNA production during early meiosis in mouse testes. Mol Cell 50:67-81

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