Gonadotropin-releasing hormone antagonist versus progestin for the prevention of premature luteinising hormone surges in poor responders undergoing in vitro fertilisation treatment: study protocol for a randomised controlled trial

Participants will be allocated randomly into one of the two arms at a ratio of 1:1 on menstrual cycle day 3. The allocation sequence will be generated utilising computer-generated random numbers. Both investigators and participants will be aware of the allocation after ovarian stimulation. The doctors and embryologists involved in oocyte retrieval and embryo transfer are blinded to the group assignments of the participants in the trial.

All follicles more than 10 mm will be retrieved. Follicles are flushed three times at most if no cumulus oocyte complex is present. Standard insemination or ICSI is performed within 6 h of retrieval. Embryos are examined for the number and regularity of blastomeres and the degree of embryonic fragmentation on the third day. If available, two top-quality embryos (including grade I and grade II, eight-cell blastomere embryos) in the GnRH antagonist group are transferred on the third day. The remaining top-quality embryos are frozen by vitrification, while the non-top-quality embryos are cultured for an extended time. Only blastocysts with good morphology are frozen on day 5 or 6. All top-quality cleavage embryos and the cryopreserved blastocysts are recorded as viable embryos. In the PPOS group, all top-quality embryos are frozen on the third day, while the non-top-quality embryos are cultured for an extended time and cryopreserved according to the same criteria as above.

Endometrium preparation uses either mild stimulation or hormone replacement therapy. For mild stimulation frozen-thawed embryo transfer cycles, we prescribe letrozole 2.5–5 mg for 3–5 days from cycle day 3 and then monitor follicular growth via serum hormone levels and ultrasound from cycle day 10. At times, treatment includes a low dose of hMG (75 IU/day) to stimulate follicle growth and the endometrial lining. When the diameter of the dominant follicle is >16 mm and the endometrial thickness is > 8 mm, with E₂ > 150 pg/ml and progesterone <1.0 ng/ml, one of two procedures is performed, depending upon the LH level. If the serum LH level is <20 mIU/ml, 5000 IU of hCG is administered at night (21:00) to trigger ovulation, and the transfer of cleavage embryos is arranged for 5 days later. If the LH level is >20 mIU/ml, 5000 IU of hCG is injected the same afternoon, and the transfer is conducted 4 days later. The blastocyst transfer is arranged on the sixth or seventh day depending on serum hormone levels and ultrasound results. Dydrogesterone (Abbott Biologicals BV, the Netherlands) was administered orally at 40 mg/day and micronised progesterone capsules at 400 mg/day was administered vaginally for luteal support beginning on the third day after hCG injection.

For patients with a thin endometrium or where the frozen-thawed embryo transfer fails after stimulation cycles, hormone replacement therapy is recommended for endometrial preparation, specifically ethinyl oestradiol administered orally at 75 mcg/day from cycle day 3 onwards, which is commonly used for 14 days. Once the endometrial lining is >8 mm thick, Femoston (a yellow tablet) is administered twice per day (Abbott Healthcare Products BV, Weesp, the Netherlands), and 400 mg micronised progesterone capsules are administered daily via an intravaginal route. The time for thawing and transfer is determined on the third day after progesterone administration. The maximum number of transferred embryos is two per cycle. When pregnancy is achieved, the progesterone supplement is continued until 10 weeks of gestation.

Serum follicle-stimulating hormone (FSH), LH, oestradiol and progesterone levels are monitored during the ovarian stimulation. Hormone levels are measured via chemiluminescence (Abbott Biologicals BV, The Netherlands).

The timepoints of enrolment, intervention, data collection and follow-up are described in Fig. 2. Data collected are entered into our electronic data capture system and stored on a secure server at Shanghai Ninth People’s Hospital. An automated system for validating data against a set of predefined rules will query investigators regarding data that are invalid, illogical or incomplete. Data elements critical to the primary aim of this trial are double-checked to confirm the accuracy of the data entered compared with the source documents.

We will utilise an intention-to-treat approach with a chi-square test to examine differences in the incidence of premature LH surges. Secondary efficacy parameters and safety parameters will be analysed using a chi-square test for enumeration data and Student’s t test for measurement data. p < 0.05 is considered as a significant difference.

The study was conceived and designed in 2016. The registry number is ChiCTR-IPR-17010906 and it was registered on 18 March 2017 (http://​www.​chictr.​org.​cn/​showproj.​aspx?​proj=​11024). The first participant was randomised on 20 March 2017. We will complete recruitment in July 2018, and patient follow-ups will be ongoing. This protocol, version 2, was approved on 12 January 2017.