Estrogen Receptor {beta} Expression and Apoptosis of Spermatocytes of Mice Overexpressing a Rat Androgen-Binding Protein Transgene

doi:10.1095/biolreprod.103.025619

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BOR - Papers in Press, published online ahead of print June 23, 2004.
Biol Reprod 2004, 10.1095/biolreprod.103.025619

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Submitted November 20, 2003
Returned for revision December 5, 2003
Accepted June 17, 2004

Testis

Estrogen Receptor ${beta}$ Expression and Apoptosis of Spermatocytes of Mice Overexpressing a Rat Androgen-Binding Protein Transgene

David M. Selva , Oscar M. Tirado , Nuria Toràn , Carlos A. Suárez-Quian , Jaume Reventos , and Francina Munell ^*

^* To whom correspondence should be addressed. E-mail: fmunell{at}vhebron.net.

Abstract
Progression of the first meiotic division in male germ cellsis regulated by a variety of factors, including androgens andpossibly estrogens. When this regulation fails, meiosis is arrestedand primary spermatocytes degenerate by apoptosis. Earlier studiesshowed that over-expression of rat androgen-binding protein(ABP) in the testis of transgenic mice results in a partialmeiotic arrest and apoptosis of pachytene spermatocytes. Inview of the recent localization of estrogen receptor ${beta}$ (ER ${beta}$ ) inprimary spermatocytes and data suggesting the ability of ER ${beta}$ to repress cellular proliferation, we tested the hypothesisthat variations in the testicular steroid micro-environmentcaused by excess ABP produce changes in ER ${beta}$ expression in this cellulartype that could be associated to the meiotic arrest and, eventually,to the induction of germ cell apoptosis observed in the ABPtransgenic mice. Increased levels of ER ${beta}$ mRNA and protein weredemonstrated in the testis of rat ABP transgenic mice comparedto non-transgenic littermates by reverse transcriptase-polymerasechain reaction (RT-PCR) experiments, Northern blotting and WesternBlotting. The major differences were found when isolated germcells of transgenic and non-transgenic littermates were analyzedby RT-PCR. In keeping with this finding, ER ${beta}$ was strongly immunolabeledin pachytene spermatocytes of rat ABP transgenic mice and localizedin tubular stages in which TUNEL labeling was maximal. Confocalmicroscopy analysis of a fluorescent TUNEL assay and ER ${beta}$ immunohistochemistryrevealed that degenerating pachytene spermatocytes over-expressedER ${beta}$ . The present results are consistent with the interpretationthat ER ${beta}$ is associated with the events that regulate negativelythe progression of meiosis or that lead to spermatocyte apoptosis.

Key words: Male Reproductive Tract • Testis • Apoptosis • Estradiol receptor • Spermatogenesis

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