Literature DB >> 16423876

Testosterone regulates FGF-2 expression during testis maturation by an IRES-dependent translational mechanism.

Irma G Gonzalez-Herrera1, Leonel Prado-Lourenco, Frédéric Pileur, Caroline Conte, Aurélie Morin, Florence Cabon, Hervé Prats, Stephan Vagner, Francis Bayard, Sylvie Audigier, Anne-Catherine Prats.   

Abstract

Spermatogenesis is a complex process involving cell proliferation, differentiation, and apoptosis. Fibroblast growth factor 2 (FGF-2) is involved in testicular function, but its role in spermatogenesis has not been fully documented. The control of FGF-2 expression particularly occurs at the translational level, by an internal ribosome entry site (IRES)-dependent mechanism driving the use of alternative initiation codons. To study IRES activity regulation in vivo, we have developed transgenic mice expressing a bicistronic construct coding for two luciferase genes. Here, we show that the FGF-2 IRES is age-dependently activated in mouse testis, whereas EMCV and c-myc IRESs are not. Real-time PCR confirms that this regulation is translational. By using immunohistological techniques, we demonstrate that FGF-2 IRES stimulation occurs in adult, but not in immature, type-A spermatogonias. This is correlated with activation of endogenous FGF-2 expression in spermatogonia; whereas FGF-2 mRNA transcription is known to decrease in adult testis. Interestingly, the FGF-2 IRES activation is triggered by testosterone and is partially inhibited by siRNA directed against the androgen receptor. Two-dimensional analysis of proteins bound to the FGF-2 mRNA 5'UTR after UV cross-linking reveals that testosterone treatment correlates with the binding of several proteins. These data suggest a paracrine loop where IRES-dependent FGF-2 expression, stimulated by Sertoli cells in response to testosterone produced by Leydig cells, would in turn activate Leydig function and testosterone production. In addition, nuclear FGF-2 isoforms could be involved in an intracrine function of FGF-2 in the start of spermatogenesis, mitosis, or meiosis initiation. This report demonstrates that mRNA translation regulation by an IRES-dependent mechanism participates in a physiological process.

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Year:  2006        PMID: 16423876     DOI: 10.1096/fj.04-3314fje

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  22 in total

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4.  Involvement of FGF9/16/20 subfamily in female germ cell development of the Nile tilapia, Oreochromis niloticus.

Authors:  Yun-Lv Sun; Sheng Zeng; Kai Ye; Chao Yang; Ming-Hui Li; Bao-Feng Huang; Li-Na Sun; Lin-Yan Zhou; De-Shou Wang
Journal:  Fish Physiol Biochem       Date:  2012-03-27       Impact factor: 2.794

Review 5.  Internal ribosome entry site-based vectors for combined gene therapy.

Authors:  Edith Renaud-Gabardos; Fransky Hantelys; Florent Morfoisse; Xavier Chaufour; Barbara Garmy-Susini; Anne-Catherine Prats
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Review 7.  High molecular weight FGF2: the biology of a nuclear growth factor.

Authors:  K Chlebova; V Bryja; P Dvorak; A Kozubik; W R Wilcox; P Krejci
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8.  Unexpected requirement for a binding partner of the syntaxin family in phagocytosis by murine testicular Sertoli cells.

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9.  Potent activation of FGF-2 IRES-dependent mechanism of translation during brain development.

Authors:  Sylvie Audigier; Janique Guiramand; Leonel Prado-Lourenco; Caroline Conte; Irma Gabriela Gonzalez-Herrera; Catherine Cohen-Solal; Max Récasens; Anne-Catherine Prats
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10.  Fibroblast growth factor 1 induced during myogenesis by a transcription-translation coupling mechanism.

Authors:  Caroline Conte; Nadera Ainaoui; Aurélie Delluc-Clavières; Marie P Khoury; Rania Azar; Françoise Pujol; Yvan Martineau; Stéphane Pyronnet; Anne-Catherine Prats
Journal:  Nucleic Acids Res       Date:  2009-06-26       Impact factor: 16.971

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