Literature DB >> 11090428

Expression and action of neurotropin-3 and nerve growth factor in embryonic and early postnatal rat testis development.

A S Cupp1, G H Kim, M K Skinner.   

Abstract

The current study examines the expression and potential actions of neurotropin-3 (NT3), nerve growth factor (NGF), and their receptors during morphological sex determination (seminiferous cord formation) and perinatal rat testis development. The expression of neurotropins and their receptors was analyzed with immunohistochemistry. Cellular localization of neurotropin ligand and receptor proteins changed during embryonic testis development. Neurotropin-3 was localized to Sertoli cells at Embryonic Day 14 (E14), was present in gonocytes at Postnatal Day 0 (P0), and after birth became localized to the interstitium and Sertoli cells (P3-P5). The expression of trk C (the high affinity receptor for NT3) was localized to mesonephric ducts and cells surrounding the cords (E14-E18). In addition, Sertoli cells and preperitubular cells surrounding the cords at E14 also stained for trk C. Neurotropin-3 was expressed in gonocytes and Sertoli cells at P0-P5. Nerve growth factor was detected in Sertoli cells at E14, was clearly in Sertoli and interstitial cells at E16 and E18, and in Sertoli, germ, and interstitial cells from P0-P5. The expression of trk A (the high affinity receptor for NGF) was located in Sertoli and interstitial cells at E16-P5. To determine the actions of neurotropins during embryonic and perinatal testis development, experiments were conducted on E13 and P0 testis. Antisense oligonucleotide experiments with NT3 were used on E13 testis organ cultures to determine effects on seminiferous cord formation. Cord formation was inhibited in 40% of the organ cultures treated with the antisense NT3 oligonucleotides, while no inhibition was observed with sense oligonucleotides. In P0 testis cultures, both NT3 and NGF alone and in combination stimulated thymidine incorporation into DNA. Therefore, the neurotropins are involved in embryonic morphological events (cord formation; NT3) and in growth of the perinatal testis (P0; NT3 and NGF). To define further the growth effects of neurotropins on testis development, expression of transforming growth factor alpha and beta (TGF alpha and TGF beta) were examined in response to neurotropins. The P0 testis cultures were treated with neurotropins, and expression of mRNA for TGF alpha and TGF beta was analyzed utilizing a quantitative reverse transcription-polymerase chain reaction assay. Nerve growth factor and NT3 alone or in combination inhibited expression of mRNA for TGF alpha while NT3 increased mRNA expression of epidermal growth factor receptor. The combination treatment of neurotropins inhibited expression of TGF beta 1 and increase expression of TGF beta 3. In summary, observations suggest that NT3, NGF, trk A, and trk C are localized to cells critical to seminiferous cord formation and appear to be important regulators of morphological sex determination. In addition to these morphological effects, both NT3 and NGF stimulate P0 testis growth and may elicit their action through altering the expression of locally produced growth factors such as TGF alpha and TGF beta. Taken together these results suggest that neurotropins are regulators of paracrine cell-cell interactions that result in morphological sex determination and perinatal testis growth.

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Year:  2000        PMID: 11090428     DOI: 10.1095/biolreprod63.6.1617

Source DB:  PubMed          Journal:  Biol Reprod        ISSN: 0006-3363            Impact factor:   4.285


  18 in total

1.  Functional interaction between p75NTR and TrkA: the endocytic trafficking of p75NTR is driven by TrkA and regulates TrkA-mediated signalling.

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2.  Cellular localization of NGF and its receptors trkA and p75LNGFR in male reproductive organs of the Japanese monkey, Macaca fuscata fuscata.

Authors:  Wanzhu Jin; Koji Y Arai; Keiko Shimizu; Chihiro Kojima; Mariko Itoh; Gen Watanabe; Kazuyoshi Taya
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3.  Regulation of the gonadal transcriptome during sex determination and testis morphogenesis: comparative candidate genes.

Authors:  Tracy M Clement; Matthew D Anway; Mehmet Uzumcu; Michael K Skinner
Journal:  Reproduction       Date:  2007-09       Impact factor: 3.906

Review 4.  How to make a gonad: cellular mechanisms governing formation of the testes and ovaries.

Authors:  E K Ungewitter; H H-C Yao
Journal:  Sex Dev       Date:  2012-05-16       Impact factor: 1.824

5.  Alterations in the developing testis transcriptome following embryonic vinclozolin exposure.

Authors:  Tracy M Clement; Marina I Savenkova; Matthew Settles; Matthew D Anway; Michael K Skinner
Journal:  Reprod Toxicol       Date:  2010-06-08       Impact factor: 3.143

6.  KDR-LacZ-expressing cells are involved in ovarian and testis-specific vascular development, suggesting a role for VEGFA in the regulation of this vasculature.

Authors:  Rebecca C Bott; Debra T Clopton; Anna M Fuller; Ryann M McFee; Ningxia Lu; Renee M McFee; Andrea S Cupp
Journal:  Cell Tissue Res       Date:  2010-09-17       Impact factor: 5.249

7.  SRY directly regulates the neurotrophin 3 promoter during male sex determination and testis development in rats.

Authors:  Tracy M Clement; Ramji K Bhandari; Ingrid Sadler-Riggleman; Michael K Skinner
Journal:  Biol Reprod       Date:  2011-04-20       Impact factor: 4.285

8.  Effects of increased nerve growth factor plasma levels on the expression of TrkA and p75 in rat testicles.

Authors:  M B Levanti; A Germanà; F de Carlos; E Ciriaco; J A Vega; G Germanà
Journal:  J Anat       Date:  2006-03       Impact factor: 2.610

Review 9.  A proposed role for VEGF isoforms in sex-specific vasculature development in the gonad.

Authors:  R C Bott; D T Clopton; A S Cupp
Journal:  Reprod Domest Anim       Date:  2008-07       Impact factor: 2.005

10.  The expression of neurotrophins and their receptors in the prenatal and adult human testis: evidence for functions in Leydig cells.

Authors:  Dieter Müller; Michail S Davidoff; Oliver Bargheer; Hans-J Paust; Wolfgang Pusch; Yvetta Koeva; Davor Jezek; Adolf F Holstein; Ralf Middendorff
Journal:  Histochem Cell Biol       Date:  2006-02-07       Impact factor: 4.304

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