Our long-term goal is to study the biology of spermatogonial stem cells, the A/single spermatogonia. There is great interest in the A/single spermatogonia because of their importance for understanding basic mechanisms of cell self-renewal versus differentiation, for the treatment of infertility, for the development of contraceptives and for the understanding of the etiology of testicular cancer, in particular seminoma. However, studies on the biology of these cells have been severely hampered because their number is low, no unique marker exists and it has been difficult to physically separate them from the other more mature spermatogonia. We recently developed a method that allows us to isolate pure populations of A/single spermatogonia, and we have started to study their behavior in vitro. Using microarrays, we also have analyzed the transcriptional program of the A/single spermatogonia in the presence of glial cell line-derived neurotrophic factor (GDNF), a growth factor produced by Sertoli cells. In the first aim, we will isolate Asingle spermatogonia and evaluate their clonogenic potential by germ cell transplantations. In the second aim, we will determine which signaling pathways are induced by GDNF, leading to Asingle spermatogonia self-renewal or differentiation. In the third aim, we will study how GDNF interacts with other growth factors/receptors to promote self-renewal or differentiation. In summary, this line of work will expand our knowledge of the functional characteristics of the A/single spermatogonia and give us better insight into the molecular mechanisms that drive the first steps of spermatogenesis. In particular, the role of the growth factor GDNF in regulating self-renewal and/or differentiation will be elucidated.

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
7R01HD044543-04
Application #
7333285
Study Section
Cellular, Molecular and Integrative Reproduction Study Section (CMIR)
Program Officer
Rankin, Tracy L
Project Start
2004-12-01
Project End
2009-11-30
Budget Start
2006-12-03
Budget End
2007-11-30
Support Year
4
Fiscal Year
2007
Total Cost
$295,832
Indirect Cost
Name
University of Illinois Urbana-Champaign
Department
Veterinary Sciences
Type
Schools of Veterinary Medicine
DUNS #
041544081
City
Champaign
State
IL
Country
United States
Zip Code
61820
Garcia, T X; Hofmann, M C (2015) Regulation of germ line stem cell homeostasis. Anim Reprod 12:35-45
Garcia, Thomas Xavier; Farmaha, Jaspreet Kaur; Kow, Sean et al. (2014) RBPJ in mouse Sertoli cells is required for proper regulation of the testis stem cell niche. Development 141:4468-78
Garcia, Thomas X; Costa, Guilherme M J; França, Luiz R et al. (2014) Sub-acute intravenous administration of silver nanoparticles in male mice alters Leydig cell function and testosterone levels. Reprod Toxicol 45:59-70
Garcia, Thomas Xavier; DeFalco, Tony; Capel, Blanche et al. (2013) Constitutive activation of NOTCH1 signaling in Sertoli cells causes gonocyte exit from quiescence. Dev Biol 377:188-201
Garcia, Thomas Xavier; Hofmann, Marie-Claude (2013) NOTCH signaling in Sertoli cells regulates gonocyte fate. Cell Cycle 12:2538-45
Lucas, Benjamin E G; Fields, Christopher; Joshi, Neeraj et al. (2012) Mono-(2-ethylhexyl)-phthalate (MEHP) affects ERK-dependent GDNF signalling in mouse stem-progenitor spermatogonia. Toxicology 299:10-9
Campos-Junior, Paulo Henrique A; Costa, Guilherme M J; Lacerda, Samyra M S N et al. (2012) The spermatogonial stem cell niche in the collared peccary (Tayassu tajacu). Biol Reprod 86:155, 1-10
Costa, Guilherme M J; Avelar, Gleide F; Rezende-Neto, Jose V et al. (2012) Spermatogonial stem cell markers and niche in equids. PLoS One 7:e44091
Garcia, Thomas; Hofmann, Marie-Claude (2012) Isolation of undifferentiated and early differentiating type A spermatogonia from Pou5f1-GFP reporter mice. Methods Mol Biol 825:31-44
Waheeb, R; Hofmann, M-C (2011) Human spermatogonial stem cells: a possible origin for spermatocytic seminoma. Int J Androl 34:e296-305; discussion e305

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