4.5 Article

Characterization and Expression of the Nuclear Progestin Receptor in Zebrafish Gonads and Brain

期刊

BIOLOGY OF REPRODUCTION
卷 82, 期 1, 页码 112-122

出版社

OXFORD UNIV PRESS INC
DOI: 10.1095/biolreprod.109.078527

关键词

hypothalamus; nuclear progestin receptor; oocyte; ovarian follicle; ovary; pgr; PR; progesterone; progesterone receptor; testis; zebrafish

资金

  1. National Science Foundation [IBN-0315349, OISE-0813146]
  2. East Carolina University Research and Creative Activity [2003-2010]
  3. East Carolina University Thomas Harriot College of Arts and Sciences Research
  4. East Carolina University Division of Research & Graduate Studies Research 2007 Development Award
  5. National Institutes of Health [ESO12961]
  6. Agence Nationale de la Recherche [2008-11]
  7. Centre National de la Recherche Scientifique

向作者/读者索取更多资源

The zebrafish nuclear progestin receptor (nPR; official symbol PGR) was identified and characterized to better understand its role in regulating reproduction in this well-established teleost model. A full-length cDNA was identified that encoded a 617-amino acid residue protein with high homology to PGRs in other vertebrates, and contained five domains characteristic of nuclear steroid receptors. In contrast to the multiplicity of steroid receptors often found in euteleosts and attributed to probable genome duplication, only a single locus encoding the full-length zebrafish pgr was identified. Cytosolic proteins from pgr-transfected cells showed a high affinity (K-d = 2 nM), saturable, single-binding site specific for a native progestin in euteleosts, 4-pregnen-17,20beta-diol-3-one (17,20beta-DHP). Both 17,20beta-DHP and progesterone were potent inducers of transcriptional activity in cells transiently transfected with pgr in a dual luciferase reporter assay, whereas androgens and estrogens had little potency. The pgr transcript and protein were abundant in the ovaries, testis, and brain and were scarce or undetectable in the intestine, muscle, and gills. Further analyses indicate that Pgr was expressed robustly in the preoptic region of the hypothalamus in the brain; proliferating spermatogonia and early spermatocytes in the testis; and in follicular cells and early-stage oocytes (stages I and II), with very low levels within maturationally competent late-stage oocytes (IV) in the ovary. The localization of Pgr suggests that it mediates progestin regulation of reproductive signaling in the brain, early germ cell proliferation in testis, and ovarian follicular functions, but not final oocyte or sperm maturation.

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