GnRH agonist for triggering final oocyte maturation in the GnRH antagonist ovarian hyperstimulation protocol: a systematic review and meta-analysis

doi:10.1093/humupd/dmi045

Human Reproduction Update Advance Access published online on October 27, 2005
Human Reproduction Update, doi:10.1093/humupd/dmi045

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© The Author 2005. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org
Received May 23, 2005
Revised July 28, 2005
Accepted September 27, 2005

Article

GnRH agonist for triggering final oocyte maturation in the GnRH antagonist ovarian hyperstimulation protocol: a systematic review and meta-analysis

G. Griesinger ¹^*, K. Diedrich ¹, P. Devroey ², and E.M. Kolibianakis ²

¹ Department of Obstetrics and Gynecology, University Clinic of Schleswig-Holstein, Campus Luebeck, Luebeck, Germany
² Centre of Reproductive Medicine, Dutch Speaking, Brussels Free University, Brussels, Belgium

^* To whom correspondence should be addressed.
G. Griesinger, E-mail: georg.griesinger{at}frauenklinik.uni-luebeck.de

Abstract

Triggering final oocyte maturation with GnRH agonist duringovarian stimulation is feasible when inhibition of prematureLH surge is performed with GnRH antagonists, and we aimed tosystematically collate evidence on the clinical efficacy ofGnRH agonist triggering in patients undergoing assisted reproductionin GnRH antagonist protocols. Twenty-three publications wereidentified by a comprehensive literature search that includedPubMed, Embase and the Cochrane Library. Three publicationsout of 23 fulfilled the inclusion criteria for meta-analysis,which were (i) prospective, randomized controlled study design;(ii) stimulation with gonadotropins for induction of multifolliculardevelopment; (iii) suppression of endogenous LH by a GnRH antagonist;(iv) triggering of final oocyte maturation with GnRH agonist;(v) control group randomized to receive HCG for final oocytematuration and (vi) any means of luteal phase support otherthan HCG. The participants were normoovulatory women undergoingIVF. The outcomes assessed were clinical pregnancy per randomizedpatient; number of oocytes retrieved; proportion of metaphaseII oocytes; fertilization rate; embryo quality score; firsttrimester abortion rate; ovarian hyperstimulation syndrome (OHSS)incidence. Results are presented as combined standardized differencesof the mean and combined odds ratios, as appropriate, with 95%confidence intervals. No significant difference was found forthe number of oocytes retrieved (-0.94,-0.33-0.14), proportionof metaphase II oocytes (-0.03,-0.58-0.52), fertilization rate(0.15,-0.09-0.38) or embryo quality score (0.05,-0.18-0.29).No OHSS occurred in two of the studies, whereas in one studyOHSS incidence was not reported. Thus from the available data,no conclusion can be drawn as regards OHSS incidence after GnRHagonist triggering. In comparison to HCG, GnRH agonist administrationis associated with a significantly reduced likelihood of achievinga clinical pregnancy (0.21, 0.05-0.84;P=0.03). The odds of firsttrimester pregnancy loss is increased after GnRH agonist triggering;however, the confidence interval crosses unity (11.51,0.95-138.98;P=0.05). In conclusion, the use of GnRH agonist to trigger finaloocyte maturation in IVF, where inhibition of premature LH surgeis achieved with GnRH antagonists, yields a number of oocytescapable to undergo fertilization and subsequent embryonic cleavage,which is comparable to that achieved with HCG. However, thelikelihood of an ongoing clinical pregnancy after GnRH agonisttriggering is significantly lower as compared to standard HCGtreatment.

Keywords: GnRH agonist/GnRH antagonist/meta-analysis/oocyte maturation.

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