Abstract

The long-term goal of these studies is to determine the mechanisms that regulate development of germ cells in the male. This is being approached by identifying genes that are expressed specifically in male germ cells and are up-regulated during particular phases of male germ cell development. These are referred to as chauvinist genes because male germ cells favor their expression with strong prejudice. They include germ cell homologue genes, unique genes, and genes expressing unique transcripts. Germ cell homologue genes are expressed only in spermatogenic cells, but are closely related to other genes expressed in somatic cells. One of these is glyceraldehyde 3-phosphate dehydrogenase (Gapd-s), likely to be important in male fertility and reproductive toxicology. The GAPD-S enzyme is """"""""off"""""""" in spermatids and """"""""on"""""""" in sperm and has a key role in regulating the generation of ATP required for fertilization. The expression of the Gapd-s mRNA and GAPD-S protein have been determined, the minimum promoter region required for transcription in transgenic mice has been identified, and the phenotype produced by a knockout of the Gapd-s gene is being determined. Studies are also underway to produce targeted mutations in three unique genes that are expressed only in spermatogenic cells and lack somatic cell isoforms. These genes encode proteins believed to have critical roles in sperm-egg binding (fertilin beta), spermatid nuclear condensation (protamine 1), and flagellar structural integrity (Fscl). The fertilin beta protein is a sperm surface component that has metalloprotease and disintegrin domains, and binds specifically to alpha1beta6 integrin on the egg surface. Protamine 1 is a highly basic protein that replaces histones during the compaction of DNA in the forming sperm head. Fscl is a major cytoskeletal component of the sperm flagellum. Mutations in the genes are expected to produce disruption of sperm formation or fertilization in homozygous male mice. The predicted phenotypes are similar to conditions observed in some infertile men and the results will be valuable both for understanding the development and function of sperm and for determining the possible roles of mutations in these genes in human infertility.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Intramural Research (Z01)
Project #
1Z01ES070076-10
Application #
2574443
Study Section
Special Emphasis Panel (LRDT)
Project Start
Project End
Budget Start
Budget End
Support Year
10
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
National Institute of Environmental Health Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Busada, Jonathan T; Velte, Ellen K; Serra, Nicholas et al. (2016) Rhox13 is required for a quantitatively normal first wave of spermatogenesis in mice. Reproduction 152:379-88
Nakamura, Noriko; Dai, Qunsheng; Williams, Jason et al. (2013) Disruption of a spermatogenic cell-specific mouse enolase 4 (eno4) gene causes sperm structural defects and male infertility. Biol Reprod 88:90
Odet, Fanny; Gabel, Scott; London, Robert E et al. (2013) Glycolysis and mitochondrial respiration in mouse LDHC-null sperm. Biol Reprod 88:95
Geyer, Christopher B; Saba, Rie; Kato, Yuzuru et al. (2012) Rhox13 is translated in premeiotic germ cells in male and female mice and is regulated by NANOS2 in the male. Biol Reprod 86:127
Odet, Fanny; Gabel, Scott A; Williams, Jason et al. (2011) Lactate dehydrogenase C and energy metabolism in mouse sperm. Biol Reprod 85:556-64
Danshina, Polina V; Geyer, Christopher B; Dai, Qunsheng et al. (2010) Phosphoglycerate kinase 2 (PGK2) is essential for sperm function and male fertility in mice. Biol Reprod 82:136-45
Geyer, Christopher B; Inselman, Amy L; Sunman, Jeffrey A et al. (2009) A missense mutation in the Capza3 gene and disruption of F-actin organization in spermatids of repro32 infertile male mice. Dev Biol 330:142-52
Zhang, Zhibing; Shen, Xuening; Gude, David R et al. (2009) MEIG1 is essential for spermiogenesis in mice. Proc Natl Acad Sci U S A 106:17055-60
Da Ros, Vanina G; Maldera, Julieta A; Willis, William D et al. (2008) Impaired sperm fertilizing ability in mice lacking Cysteine-RIch Secretory Protein 1 (CRISP1). Dev Biol 320:12-8
Odet, Fanny; Duan, Chongwen; Willis, William D et al. (2008) Expression of the gene for mouse lactate dehydrogenase C (Ldhc) is required for male fertility. Biol Reprod 79:26-34

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