Abstract

The proposed research uses the genetic analysis of C. elegans to address two fundamental questions in germline development: how is the decision to either proliferate or enter the meiotic pathway executed? And how are meiotic prophase progression and gametogenesis controlled and coordinated? Disruption of these processes can result in germline tumor formation, sterility and aneuploid gemetes. We have identified mutations that cause germline tumorigenesis by two different mechanisms. Gain-of- function mutations in the glp-I and let-42 genes lead to tumorigenesis by preventing germline stem cells from exiting mitosis and entering the meiotic pathway. In contrast, loss-of- function mutations in the gld-I gene cause tumor formation by disrupting meiotic prophase progression and oogenesis. In animals lacking gld-1 activity, germ cells that would normally develop into oocytes enter and progress through meiotic prophase normally until the early pachytene stage, when they exit the meiotic pathway and return to a proliferative cell cycle. We have shown that this return to mitosis is dependent on the activity of MAP kinase. We have also identified a new gene, pex-2, that is important for meiotic prophase progression. glp-1, let-42 and gld-1 are evolutionarily conserved. GLP-1 is related to the Notch family of receptors, which includes the human TAN-1 proto-oncogene product. Let-42 shows similarity to an uncharacterized human cDNA. GLD-1, a putative RNA binding protein, shares homology with the mouse Quaking protein and the human Sam68 protein.
The specific aims of this proposal are to: A) identify genes that negatively regulate mitosis or positively regulate entry into meiosis by screening for enhancers of a weak glp-1 (gf) mutation; B) analyze the normal role of let-42 in germline proliferation; C) identify regulators, cofactors and RNA targets of GLD-1 and investigate the role of the MAP kinase pathway in germline tumorigenesis; and D) determine how pex-2 promotes meiotic prophase progression. The proposed studies relate to general aspects of biology and medicine. They will provide insights into: the regulation of mitosis; the control of entry into and progression through meiotic prophase; and the functioning and regulation of Notch family receptors, the MAP kinase signalling pathway, LET-42 and the GLD-1/Quaking/Sam68 subfamily of RNA binding proteins. This work may also provide new information about the cellular mechanisms that underlie human germline cancers.

  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 #
5R01HD025614-10
Application #
2838744
Study Section
Genetics Study Section (GEN)
Program Officer
Tasca, Richard J
Project Start
1979-04-01
Project End
2000-11-30
Budget Start
1998-12-01
Budget End
1999-11-30
Support Year
10
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Genetics
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Miller, M A; Nguyen, V Q; Lee, M H et al. (2001) A sperm cytoskeletal protein that signals oocyte meiotic maturation and ovulation. Science 291:2144-7
Kuwabara, P E; Lee, M H; Schedl, T et al. (2000) A C. elegans patched gene, ptc-1, functions in germ-line cytokinesis. Genes Dev 14:1933-44
Clifford, R; Lee, M H; Nayak, S et al. (2000) FOG-2, a novel F-box containing protein, associates with the GLD-1 RNA binding protein and directs male sex determination in the C. elegans hermaphrodite germline. Development 127:5265-76
Berry, L W; Westlund, B; Schedl, T (1997) Germ-line tumor formation caused by activation of glp-1, a Caenorhabditis elegans member of the Notch family of receptors. Development 124:925-36
Kloek, A P; McCarter, J P; Setterquist, R A et al. (1996) Caenorhabditis globin genes: rapid intronic divergence contrasts with conservation of silent exonic sites. J Mol Evol 43:101-8
Iwasaki, K; McCarter, J; Francis, R et al. (1996) emo-1, a Caenorhabditis elegans Sec61p gamma homologue, is required for oocyte development and ovulation. J Cell Biol 134:699-714
Crowder, C M; Shebester, L D; Schedl, T (1996) Behavioral effects of volatile anesthetics in Caenorhabditis elegans. Anesthesiology 85:901-12
Jones, A R; Francis, R; Schedl, T (1996) GLD-1, a cytoplasmic protein essential for oocyte differentiation, shows stage- and sex-specific expression during Caenorhabditis elegans germline development. Dev Biol 180:165-83
Francis, R; Maine, E; Schedl, T (1995) Analysis of the multiple roles of gld-1 in germline development: interactions with the sex determination cascade and the glp-1 signaling pathway. Genetics 139:607-30
Francis, R; Barton, M K; Kimble, J et al. (1995) gld-1, a tumor suppressor gene required for oocyte development in Caenorhabditis elegans. Genetics 139:579-606

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