TY - JOUR
T1 - Testosterone for Poor Ovarian Responders
T2 - Lessons From Ovarian Physiology
AU - Polyzos, Nikolaos P
AU - Davis, Susan R
AU - Drakopoulos, Panagiotis
AU - Humaidan, Peter
AU - De Geyter, Christian
AU - Vega, Antonio Gosálvez
AU - Martinez, Francisca
AU - Evangelou, Evangelos
AU - van de Vijver, Arne
AU - Smitz, Johan
AU - Tournaye, Herman
AU - Barri, Pedro
AU - T-TRANSPORT Investigators Group
N1 - © The Author(s) 2016.
PY - 2018/7
Y1 - 2018/7
N2 - Testosterone, an androgen that directly binds to the androgen receptor, has been shown in previous small randomized controlled trials to increase the reproductive outcomes of poor ovarian responders. In most of these studies, transdermal testosterone in relatively high doses was administered before ovarian stimulation with a duration varying from 5 to 21 days. Nevertheless, the key question to be asked is whether, based on ovarian physiology and testosterone pharmacokinetics, a short course of testosterone administration of more than 10 mg could be expected to have any beneficial effect on reproductive outcome. The rationale for asking this question lies in the existing scientific evidence derived from basic research and animal studies regarding the action of androgens during folliculogenesis, showing that their main effect in follicular development is defined during the earlier developmental stages. In addition, extreme testosterone excess is not only likely to induce adverse events but has also the potential to be ineffective and even detrimental. Thus, evidence from clinical studies is not enough to either "reopen" or "close" the "androgen chapter" in poor responders, mainly because the short administration and the high dose of testosterone is not in line with the ovarian actions of androgens and the presence of androgen receptors during follicular development.
AB - Testosterone, an androgen that directly binds to the androgen receptor, has been shown in previous small randomized controlled trials to increase the reproductive outcomes of poor ovarian responders. In most of these studies, transdermal testosterone in relatively high doses was administered before ovarian stimulation with a duration varying from 5 to 21 days. Nevertheless, the key question to be asked is whether, based on ovarian physiology and testosterone pharmacokinetics, a short course of testosterone administration of more than 10 mg could be expected to have any beneficial effect on reproductive outcome. The rationale for asking this question lies in the existing scientific evidence derived from basic research and animal studies regarding the action of androgens during folliculogenesis, showing that their main effect in follicular development is defined during the earlier developmental stages. In addition, extreme testosterone excess is not only likely to induce adverse events but has also the potential to be ineffective and even detrimental. Thus, evidence from clinical studies is not enough to either "reopen" or "close" the "androgen chapter" in poor responders, mainly because the short administration and the high dose of testosterone is not in line with the ovarian actions of androgens and the presence of androgen receptors during follicular development.
KW - Infertility
KW - Poor ovarian response
KW - Poor responders
KW - Testosterone
UR - http://www.scopus.com/inward/record.url?scp=85043469684&partnerID=8YFLogxK
U2 - 10.1177/1933719116660849
DO - 10.1177/1933719116660849
M3 - Article
C2 - 27489169
SN - 1933-7191
VL - 25
SP - 980
EP - 982
JO - Reproductive Sciences
JF - Reproductive Sciences
IS - 7
ER -