Abstract

The experiments proposed here address the interdependency of genetic events of meiotic prophase with the regulation of the meiotic cell cycle during mammalian spermatogenesis. This work is inspired by recent observations that meiotic metaphase can be rapidly and precociously induced in midprophase mouse spermatocytes in culture. The fundamental hypothesis to be tested is that the spermatocyte develops competency to condense chiasmate bivalent metaphase chromosomes concomitant with the appearance of the tripartite synaptonemal complex, and that competence requires both effective chromosome pairing and function of the synaptonemal complex. Key to this work is the availability of a novel system for induction of meiotic metaphase in spermatocytes in vitro. To test this hypothesis, zygotene and early pachytene spermatocytes will be used in a competency assay and genetic mutants will be used to assess the role of chromosome pairing and the synaptonemal complex. This work will also test the hypothesis that spermatocyte competence to condense metaphase chromosomes also depends on accumulation and activation of proteins that mediate the cell-cycle transition. Roles of critical regulators of chromosome condensation and the cell cycle, topoisomerase Il, MPF, MAPK, and phosphatases, will be assessed by biochemical assays to determine presence and activity of these proteins in noncompetent, competent, and meiotic metaphase cells. Additionally, various methods, including transfer of spermatocyte nuclei into maturing mouse oocytes, will be used to induce pachytene spermatocytes to undergo meiotic divisions in order to determine when competence to segregate chromosomes during the meiotic divisions arises. Segregation will be monitored by a fluorescence in situ hybridization (FISH) assay that reliably assesses fidelity of chromosome segregation. The results of these experiments will provide new and crucial information about mechanisms regulating the spermatogenic cell cycle, as well as relate cell cycle to meiotic chromosome segregation. The latter is of importance in the etiology of aneuploidy, a major contributor to human early pregnancy failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD033816-03
Application #
2673939
Study Section
Reproductive Biology Study Section (REB)
Project Start
1996-09-01
Project End
2000-08-31
Budget Start
1998-09-01
Budget End
1999-08-31
Support Year
3
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
University of Tennessee Knoxville
Department
Biochemistry
Type
Schools of Arts and Sciences
DUNS #
City
Knoxville
State
TN
Country
United States
Zip Code
37996

  Publications

Hwang, Grace; Sun, Fengyun; O'Brien, Marilyn et al. (2017) SMC5/6 is required for the formation of segregation-competent bivalent chromosomes during meiosis I in mouse oocytes. Development 144:1648-1660
Ball, Robyn L; Fujiwara, Yasuhiro; Sun, Fengyun et al. (2016) Regulatory complexity revealed by integrated cytological and RNA-seq analyses of meiotic substages in mouse spermatocytes. BMC Genomics 17:628
Cheng, Albert W; Jillette, Nathaniel; Lee, Phoebe et al. (2016) Casilio: a versatile CRISPR-Cas9-Pumilio hybrid for gene regulation and genomic labeling. Cell Res 26:254-7
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
La Salle, Sophie; Palmer, Kristina; O'Brien, Marilyn et al. (2012) Spata22, a novel vertebrate-specific gene, is required for meiotic progress in mouse germ cells. Biol Reprod 86:45
Jordan, Philip W; Karppinen, Jesse; Handel, Mary A (2012) Polo-like kinase is required for synaptonemal complex disassembly and phosphorylation in mouse spermatocytes. J Cell Sci 125:5061-72
Fritsche, Miriam; Reinholdt, Laura G; Lessard, Mark et al. (2012) The impact of entropy on the spatial organization of synaptonemal complexes within the cell nucleus. PLoS One 7:e36282
Sun, Fengyun; Handel, Mary Ann (2011) A Mutation in Mtap2 Is Associated with Arrest of Mammalian Spermatocytes before the First Meiotic Division. Genes (Basel) 2:21-35
Sun, Fengyun; Palmer, Kristina; Handel, Mary Ann (2010) Mutation of Eif4g3, encoding a eukaryotic translation initiation factor, causes male infertility and meiotic arrest of mouse spermatocytes. Development 137:1699-707
La Salle, Sophie; Sun, Fengyun; Handel, Mary Ann (2009) Isolation and short-term culture of mouse spermatocytes for analysis of meiosis. Methods Mol Biol 558:279-97

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