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Female Fertility: What’s Testosterone Got To Do With It?

New Study Shows Male Hormones Play an Important Role; May Enhance IVF Therapy

Several fertility clinics across the country are beginning to administer testosterone, either through a patch or a gel on the skin, to increase the number of eggs produced by certain women undergoing in vitro fertilization (IVF). Women are also purchasing the over-the-counter supplement DHEA, which is converted by the body into testosterone, to boost their chances of pregnancy with IVF.

A few clinical trials support the use of testosterone given through the skin, while others have shown no benefit of DHEA – also used in attempts to slow aging and enhance muscle mass – in increasing pregnancy and birth rates in women who don’t respond well to IVF therapy. Lacking a large and convincing body of data on the topic, the jury is still out as to whether male hormones such as testosterone improve female fertility.

A new study suggests that male hormones, also called androgens, help drive the development of follicles – structures that contain and ultimately release an egg that can be fertilized by a man’s sperm. Published in the Proceedings of the National Academy of Sciences, the research also details how male hormones boost the production of follicles in mice. Authors believe the study provides potential biological targets to enhance fertility in women with diminished ovarian reserve, who produce few or no follicles in response to IVF drugs designed to boost follicle development.

“There is a raging debate in the reproductive endocrinology field about what male hormones are doing in female fertility,” said Stephen R. Hammes, M.D., Ph.D.,senior study author and professor of Endocrinology at the University of Rochester School of Medicine and Dentistry. “Our study doesn’t solve the controversy, but, along with some earlier seminal studies from other groups, it does tell us that we can’t dismiss male hormones. They might actually be doing something useful.”

Using multiple animal models and cell experiments, Hammes and lead study author Aritro Sen, Ph.D., research assistant professor of Endocrinology at the medical school found that male hormones promote follicle development in two ways. First, they prevent follicles from dying at an early stage. They do this by ramping up a molecule that stops cells from self destructing, a process called apoptosis. Hammes and Sen speculate that if a woman doesn’t have enough androgens (male hormones), more of her follicles may be dying and fewer progressing to a mature stage when they produce and release an egg.

Second, androgens make ovarian cells more sensitive to follicle-stimulating hormone or FSH, which promotes follicle growth. They do this by creating more FSH receptors – molecules on the surface of ovarian cells that jumpstart the follicle making process in response to the hormone.

“Androgens are increasing follicle growth and ensuring follicles don’t die – exactly what you want when providing fertility treatment,” noted Hammes, who is also the chief of the Division of Endocrinology and Metabolism at UR Medicine’s Strong Memorial Hospital.

When the team administered small doses of androgens to mice that were taking the equivalent of medications given to women undergoing IVF therapy, they developed more mature, egg-containing follicles than mice that didn’t receive androgens.  The androgen-treated female mice also released larger numbers of eggs with ovulation.  IVF drugs are designed to do just that, enhance ovulation – the production and discharge of an egg or eggs from the ovary. Unfortunately, these drugs aren’t always effective in women with diminished ovarian reserve.

Kathleen M. Hoeger, M.D., M.P.H., director of UR Medicine’s Strong Fertility Center, estimates that around 20 percent of the patients her team treats have diminished ovarian reserve, meaning they produce fewer follicles than estimated based on their age. Women who are 40 years or older are most likely to have diminished ovarian reserve, but it can appear in younger women as well.

“This information is important because it provides theoretical support for administering androgens to some women undergoing IVF, a practice that our fertility clinic and many others across the country have started in recent years,” said Hoeger, who is also a professor of Obstetrics and Gynecology at the School of Medicine and Dentistry. “If these data are confirmed in clinical trials, we could propose that raising low levels of androgens in a woman with diminished ovarian reserve might increase her ability to produce more and better eggs for fertilization.”

Hammes says the study calls for further clinical trials to determine whether androgens can have a positive effect on fertility when given at the right doses. And, by better understanding the biological pathways that are important for follicle development, scientists may be able to target these pathways with drugs or other interventions to improve IVF success rates.

In addition to Hammes and Sen, Hen Prizant, Allison Light, Anindita Biswas and Emily Hayes from the University of Rochester School of Medicine and Dentistry contributed to the research. Ho-Joon Lee, David Barad and Norbert Gleicher from the Center for Human Reproduction in New York also participated in the study. Funding was provided by the Foundation for Reproductive Medicine.




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2 thoughts on “Female Fertility: What’s Testosterone Got To Do With It?”

  1. This is hope for women, like myself, doing infertility treatments who have been poor responders to medicated ovarian stimulation. This is something women are discussing on http://www.fertilethoughts.com/forums and we would love to have you join us there.

    I wish this information had been available for me when I was cycling with my own eggs. I wonder if it would have made a difference between me using my own genetic material or donor eggs.

  2. Excellent study and should have helpful guidance and potential positive input and ultimate success for the infertility specialists and patients for pregnancy .
    Main author of the study Dr.Stephen R.Hammes reportedly stated that “Our study doesn’t solve the controversy, but, along with some earlier seminal studies from other groups, it does tell us that we can’t dismiss male hormones. They might actually be doing something useful.”
    He is absolutely correct `fundamentally` and he is on the target for the better outcome and results for the fertility clinics , in fact there should be no controversy on this issue that the `Testosterone` is essential hormone for healthy `ovum` production . All women normally have testosterone hormone as well as estrogen and progesterone , for men testosterone is absolutely essential for `sperm cell production-called spermatogenesis through SERTOLI cells , these cells ; Sertoli cells of male testis has both testosterone and FSH (Follicle stimulating hormone) RECEPTORS , these Sertoli cells are called ‘NURSE ‘ cells of the testes has utmost importance in differentiation and the support of spermatogenesis (sperm production) .
    And female equivalent(ANALOG) of Sertoli cells are the `GRANULOSA` cells of the female follicle in the ovaries , and the `OVULATORY` observed synergistic effect of TESTOSTERONE and FSH hormones both are very likely true these `Granulose cells of follicle in the ovaries` . Rather than direct effect on the ovum itself .
    So any synergistic stimulus of both hormones (Testosterone+FSH ) should have positive effect through GRANULOSA cells on “ the differentiation and support of Ovum” based on the knowledge we have on SERTOLI cells of male testicles and sperm production through spermatogenesis .
    http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2871953/ Direct Action through the Sertoli Cells Is Essential for Androgen Stimulation of Spermatogenesis
    http://en.wikipedia.org/wiki/Sertoli_cell Sertoli Cells
    http://www.reproduction-online.org/content/130/1/15.full

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