Abstract

An intimate physical and functional relationship exists between Sertoli cells and germ cells in testes of adult rats. Sertoli cell division occurs only during perinatal development, when the size of this population is established. This period may be of major importance in insuring production of sufficient sperm, i.e., fertility in adults. To test this, the PI will study spermatogenesis in adult rats that have either abnormally few or many Sertoli cells: the point(s) in germ cell maturation dependent on Sertoli cells will be identified and the impact of Sertoli cell population size on fertility analyzed by testing the ability of Sertoli cell-deficient rats to impregnate females. Although the PI identified FSH as a major factor regulating Sertoli cell proliferation in vivo, virtually nothing is known about how it initiates DNA synthesis in these cells, or about other possible levels of control over the size of this population. The PI will probe the events set in motion by FSH that culminate in Sertoli cell division by addressing: (1) the role of intracellular Ca++ in mediating FSH-induced Sertoli cell division; (2) the involvement of a Ca++-sensitive phosphodiesterase unique to immature Sertoli cells in the proliferative response; (3) the relationship among the position of a Sertoli cell in the cell cycle, its possession of functional FSH receptors and its ability to respond to FSH; and (4) the role of estrogen formation in promoting Sertoli cell division. The PI will also explore the possibility that testicular POMC-derived peptides, e.g., b-endorphin, exert paracrine control over Sertoli cell population size, thus modifying the effect of FSH, by testing the effect of either endorphin blockade or administration on Sertoli cell proliferation. Endorphin binding sites will be localized in the neonatal testis, and studies carried out to probe the nature, at the cellular level, of the mechanism by which this peptide suppresses FSH-stimulated Sertoli cell division. Studies are proposed in vitro to allow control of the conditions under study and in vivo to permit evaluation of the physiological significance of the findings. Data emerging from this work should provide new information on the role of Sertoli cell development in establishing fertility and yield new insights into how development of these cells may be modified in vivo, thus enlarging our understanding of fertility and infertility in males.

  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 #
5R01HD015563-07
Application #
3313171
Study Section
Reproductive Biology Study Section (REB)
Project Start
1981-09-01
Project End
1989-08-31
Budget Start
1987-09-01
Budget End
1988-08-31
Support Year
7
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Temple University
Department
Type
Schools of Medicine
DUNS #
City
Philadelphia
State
PA
Country
United States
Zip Code
19122

  Publications

Wu, Ji; Jester Jr, William F; Orth, Joanne M (2005) Short-type PB-cadherin promotes survival of gonocytes and activates JAK-STAT signalling. Dev Biol 284:437-50
Wu, J; Jester Jr, W F; Laslett, A L et al. (2003) Expression of a novel factor, short-type PB-cadherin, in Sertoli cells and spermatogenic stem cells of the neonatal rat testis. J Endocrinol 176:381-91
Laslett, A L; Li, L H; Jester Jr, W F et al. (2000) Thyroid hormone down-regulates neural cell adhesion molecule expression and affects attachment of gonocytes in Sertoli cell-gonocyte cocultures. Endocrinology 141:1633-41
Li, L H; Jester Jr, W F; Orth, J M (1998) Expression of 140-kDa neural cell adhesion molecule in developing testes in vivo and in long-term Sertoli cell-gonocyte cocultures. J Androl 19:365-73
Orth, J M; McGuinness, M P; Qiu, J et al. (1998) Use of in vitro systems to study male germ cell development in neonatal rats. Theriogenology 49:431-9
Orth, J M; Qiu, J; Jester Jr, W F et al. (1997) Expression of the c-kit gene is critical for migration of neonatal rat gonocytes in vitro. Biol Reprod 57:676-83
Pilder, S H; Olds-Clarke, P; Orth, J M et al. (1997) Hst7: a male sterility mutation perturbing sperm motility, flagellar assembly, and mitochondrial sheath differentiation. J Androl 18:663-71
Orth, J M; Jester Jr, W F; Qiu, J (1996) Gonocytes in testes of neonatal rats express the c-kit gene. Mol Reprod Dev 45:123-31
Latham, K E; Litvin, J; Orth, J M et al. (1996) Temporal patterns of A-myb and B-myb gene expression during testis development. Oncogene 13:1161-8
Orth, J M; Jester Jr, W F (1995) NCAM mediates adhesion between gonocytes and Sertoli cells in cocultures from testes of neonatal rats. J Androl 16:389-99

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