- Made available online as an Accepted Preprint 21 August 2008
- Accepted Preprint first posted online on 21 August 2008
Estrogen treatment up-regulates female genes but does not suppress all early testicular markers during rainbow trout male-to-female gonadal transdifferentiation
- Denise Vizziano-Cantonnet1,2,
- Daniel Baron2,
- Sophie Mahè2,
- Chantal Cauty2,
- Alexis Fostier2 and
- Yann Guiguen2
- 1Facultad de Ciencias, Oceanología, Iguá 4225, Montevideo 11400, Uruguay2INRA, UR1037, IFR140, SCRIBE, F-35000 Rennes, France
- (Correspondence should be addressed to Y Guiguen at INRA, France; Email: yann.guiguen{at}rennes.inra.fr)
Abstract
In non-mammalian vertebrates, estrogens are key players in ovarian differentiation, but the mechanisms by which they act remain poorly understood. The present study on rainbow trout was designed to investigate whether estrogens trigger the female pathway by activating a group of early female genes (i.e. cyp19a1, foxl2a, foxl2b, fst, bmp4, and fshb) and by repressing early testicular markers (i.e. dmrt1, nr0b1, sox9a1 and sox9a2). Feminization was induced in genetically all-male populations using 17α-ethynylestradiol (EE2, 20 mg/kg of food during 2 months). The expression profiles of 100 candidate genes were obtained by real-time RT-PCR and 45 expression profiles displayed a significant differential expression between control populations (males and females) and EE2-treated populations. These expression profiles were grouped in five temporally correlated expression clusters. The estrogen treatment induced most of the early ovarian differentiation genes (foxl2a, foxl2b, fst, bmp4, and fshb) and in particular foxl2a, which was strongly and quickly up-regulated. Simultaneously, Leydig cell genes, involved in androgen synthesis, as well as some Sertoli cell markers (amh, sox9a2) were strongly repressed. However, in contrast to our initial hypothesis, some genes considered as essential for mammalian and fish testis differentiation were not suppressed during the early process of estrogen-induced feminization (dmrt1, nr0b1, sox9a1 and pax2a) and some were even strongly up-regulated (nr0b1, sox9a1and pax2a). In conclusion, estrogens trigger male-to-female transdifferentiation by up-regulating most ovarian specific genes and this up-regulation appears to be crucial for an effective feminization, but estrogens do not concomitantly down-regulate all the testicular differentiation markers.
- Revision received 9 July 2008
- Accepted 21 August 2008
- © 2008 Society for Endocrinology