Abstract

Ovarian follicular development is dependent on hormone (estradiol and FSH) induced changes in granulosa cell function which lead to the amplication of cAMP production, cAMP binding sites and cAMP-dependent protein phosphorylation- events presumed to be required for ovulation and luteinization. Despite the importance of estradiol and FSH action in granulosa cells, the precise target sites and molecular processes regulated by these signals remain largely unknown. One protein whose content is increased at least 5-10 fold in vivo and in vitro by estradiol and FSH (and cAMP) in granulosa cells is R-II, the regulatory subunit of type II cAMP dependent protein kinase. Furthermore, recent observations indicate that granulosa cell R-II may be an ovarian specific isozyme of a multigene family. Based on these considerations we propose to use ovarian R-II as a """"""""model"""""""" protein for analyzing the molecular aspects of estradiol and FSH action in granulosa cells. Accordingly we propose to: 1) purify and characterize the hormone-regulated R-II from rat ovaries and prepare antibodies; 2) construct a rat granulosa cell gene expression library to isolate R-II cDNA; 3) determine the mechanisms by which estradiol and FSH (cAMP) regulate the synthesis of R-II; 4) determine some of the molecular events associated with granulosa cell luteinization; 5) determine the hormonal regulation of receptors for estradiol in cultured granulosa cells. These goals will be accomplished by applying to the rat granulosa cells system tools which have been developed in molecular biology. Specifically, we will isolate poly(A)+ RNA from granulosa cells, prepare a gene expression library in Gammagtll bacteriophage, identify cDNA for R-II by antibody or oligonucleotide screening, subclone the cDNA for R-II and use it as a probe to answer questions about how estradiol and cAMP act to regulate the transcription of the ovarian specific R-II gene. Two granulosa cell culture systems have been established to analyze the actions of estradiol and FSH (and cAMP) of granulosa cell function. Short-term cultures (in serum-free medium) provide a system for analyzing the induction of R-II in differentiating cells in response to FSH and low concentrations of cAMP. The long-term cultures (in low concentrations of serum) provide a system for analyzing the mechanisms by which hCG/LH and high cAMP cause luteinization and a loss of R-II. Using these approaches, we hope to understand the molecular events associated with the synergistic regulation of granulosa cell differentiation by estradiol and FSH.

  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 #
2R01HD016272-05
Application #
3313569
Study Section
Biochemical Endocrinology Study Section (BCE)
Project Start
1981-09-01
Project End
1989-06-30
Budget Start
1986-07-01
Budget End
1987-06-30
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Baylor College of Medicine
Department
Type
Schools of Medicine
DUNS #
074615394
City
Houston
State
TX
Country
United States
Zip Code
77030

  Publications

Dumesic, Daniel A; Richards, Joanne S (2013) Ontogeny of the ovary in polycystic ovary syndrome. Fertil Steril 100:23-38
Liu, Zhilin; Castrillon, Diego H; Zhou, Wei et al. (2013) FOXO1/3 depletion in granulosa cells alters follicle growth, death and regulation of pituitary FSH. Mol Endocrinol 27:238-52
Richards, J S; Fan, H-Y; Liu, Z et al. (2012) Either Kras activation or Pten loss similarly enhance the dominant-stable CTNNB1-induced genetic program to promote granulosa cell tumor development in the ovary and testis. Oncogene 31:1504-20
Richards, JoAnne S; Liu, Zhilin; Kawai, Tomoko et al. (2012) Adiponectin and its receptors modulate granulosa cell and cumulus cell functions, fertility, and early embryo development in the mouse and human. Fertil Steril 98:471-9.e1
Boerboom, Derek; Lafond, Jean-François; Zheng, Xiaofeng et al. (2011) Partially redundant functions of Adamts1 and Adamts4 in the perinatal development of the renal medulla. Dev Dyn 240:1806-14
Richards, Joanne S; Pangas, Stephanie A (2010) New insights into ovarian function. Handb Exp Pharmacol :3-27
Richards, Joanne S; Pangas, Stephanie A (2010) The ovary: basic biology and clinical implications. J Clin Invest 120:963-72
Boyer, Alexandre; Lapointe, Evelyne; Zheng, Xiaofeng et al. (2010) WNT4 is required for normal ovarian follicle development and female fertility. FASEB J 24:3010-25
Fan, Heng-Yu; Liu, Zhilin; Paquet, Marilene et al. (2009) Cell type-specific targeted mutations of Kras and Pten document proliferation arrest in granulosa cells versus oncogenic insult to ovarian surface epithelial cells. Cancer Res 69:6463-72
Lague, Marie-Noelle; Paquet, Marilene; Fan, Heng-Yu et al. (2008) Synergistic effects of Pten loss and WNT/CTNNB1 signaling pathway activation in ovarian granulosa cell tumor development and progression. Carcinogenesis 29:2062-72

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