Literature DB >> 24877631

Loss of Ntrk2/Kiss1r signaling in oocytes causes premature ovarian failure.

Mauricio D Dorfman1, Cecilia Garcia-Rudaz, Zefora Alderman, Bredford Kerr, Alejandro Lomniczi, Gregory A Dissen, Juan Manuel Castellano, David Garcia-Galiano, Francisco Gaytan, Baoji Xu, Manuel Tena-Sempere, Sergio R Ojeda.   

Abstract

Neurotrophins (NTs), once believed to be neural-specific trophic factors, are now known to also provide developmental cues to non-neural cells. In the ovary, NTs contribute to both the formation and development of follicles. Here we show that oocyte-specific deletion of the Ntrk2 gene that encodes the NTRK2 receptor (NTRK2) for neurotrophin-4/5 and brain-derived neurotrophic factor (BDNF) results in post-pubertal oocyte death, loss of follicular organization, and early adulthood infertility. Oocytes lacking NTRK2 do not respond to gonadotropins with activation of phosphatidylinositol 3-kinase (PI3K)-AKT-mediated signaling. Before puberty, oocytes only express a truncated NTRK2 form (NTRK2.T1), but at puberty full-length (NTRK2.FL) receptors are rapidly induced by the preovulatory gonadotropin surge. A cell line expressing both NTRK2.T1 and the kisspeptin receptor (KISS1R) responds to BDNF stimulation with activation of Ntrk2 expression only if kisspeptin is present. This suggests that BDNF and kisspeptin that are produced by granulosa cells (GCs) of periovulatory follicles act in concert to mediate the effect of gonadotropins on Ntrk2 expression in oocytes. In keeping with this finding, the oocytes of NTRK2-intact mice fail to respond to gonadotropins with increased Ntrk2 expression in the absence of KISS1R. Our results demonstrate that the preovulatory gonadotropin surge promotes oocyte survival at the onset of reproductive cyclicity by inducing oocyte expression of NTRK2.FL receptors that set in motion an AKT-mediated survival pathway. They also suggest that gonadotropins activate NTRK2.FL expression via a dual communication pathway involving BDNF and kisspeptin produced in GCs and their respective receptors NTRK2.T1 and KISS1R expressed in oocytes.

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Year:  2014        PMID: 24877631      PMCID: PMC4097998          DOI: 10.1210/en.2014-1111

Source DB:  PubMed          Journal:  Endocrinology        ISSN: 0013-7227            Impact factor:   4.736


  47 in total

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5.  Brain-derived neurotrophic factor: a novel human ovarian follicular protein.

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9.  Kisspeptin receptor haplo-insufficiency causes premature ovarian failure despite preserved gonadotropin secretion.

Authors:  Francisco Gaytan; David Garcia-Galiano; Mauricio D Dorfman; Maria Manfredi-Lozano; Juan M Castellano; Gregory A Dissen; Sergio R Ojeda; Manuel Tena-Sempere
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2.  Kisspeptin cell-specific PI3K signaling regulates hypothalamic kisspeptin expression and participates in the regulation of female fertility.

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3.  Ovarian kisspeptin expression is related to age and to monocyte chemoattractant protein-1.

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Authors:  Francisco Gaytan; David Garcia-Galiano; Mauricio D Dorfman; Maria Manfredi-Lozano; Juan M Castellano; Gregory A Dissen; Sergio R Ojeda; Manuel Tena-Sempere
Journal:  Endocrinology       Date:  2014-06-02       Impact factor: 4.736

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Review 7.  Comprehensive Review on Kisspeptin and Its Role in Reproductive Disorders.

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9.  The pregnant mouse uterus exhibits a functional kisspeptin/KISS1R signaling system on the day of embryo implantation.

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