Endometrial Compaction and Its Influence on Pregnancy Rate in Frozen Embryo Cycle Regimes

Sponsor

ART Fertility Clinics LLC (Other)

Overall Status

Terminated

CT.gov ID

NCT04454749

Collaborator

(none)

Enrollment

Location

3.8

Actual Duration (Months)

0.8

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

For a pregnancy to occur, an euploid embryo at blastocyst developmental stage, a receptive endometrium and the synchrony of both is crucial. Many studies lately investigated the influence of the endometrial thickness and pattern on the artificial reproductive technology (ART) outcome, however, with conflicting results.

Condition or Disease	Intervention/Treatment	Phase
Endometrial Disorder Infertility, Female IVF Pregnancy Early	Diagnostic Test: Blood test Diagnostic Test: Ultrasound

Detailed Description

Further on, the measurement of the endometrial thickness was mostly performed either on the day of final oocyte maturation in stimulated cycles with fresh embryo transfer or on the day of progesterone administration in FET cycles.

Progesterone is essential for the secretory transformation and compaction of the endometrium, prior to implantation. A recently published paper (Haas et al., 2019) however, evaluated the degree of endometrial compaction under the influence of progesterone in FET cycles and described, that a lack of certain endometrial compaction has a negative impact on the ongoing pregnancy rate. As in this study embryos of unknown ploidy status were transferred, the role of embryo ploidy on the outcome may bias the study results.

In the herein presented study protocol we aim to investigate the influence of endometrial compaction in FET cycles in which euploid embryos are transferred.

HYPOTHESIS: Lack of endometrial compaction after the start of progesterone leads to an impaired reproductive outcome.

Study Design

Study Type:

Observational

Actual Enrollment :

3 participants

Observational Model:

Cohort

Time Perspective:

Prospective

Official Title:

Endometrial Compaction and Its Influence on Pregnancy Rate in Frozen Embryo Cycle Regimes

Actual Study Start Date :

Nov 9, 2020

Actual Primary Completion Date :

Feb 25, 2021

Actual Study Completion Date :

Mar 4, 2021

Arms and Interventions

Arm	Intervention/Treatment
Stimulated cycles Ovarian stimulation will be performed by standard protocols. Stimulation medication dosage will be individualised prior to stimulation start according to the ovarian reserve parameters and during ovarian stimulation according to the ovarian response and the measured levels of E2 and progesterone (P4), in order to avoid progesterone elevation during late follicular phase. Final oocyte maturation will be achieved by administration of either 10.000 IU of hCG, 0.3 mg of GnRH agonist (Triptorelin) or dual trigger (hCG and GnRH-analogue), as soon as ≥ 3 follicles ≥ 17 mm are present. Oocyte retrieval will be carried out 36 hours after administration of the trigger. Embryos will undergo PGT-A at blastocyst stage and be vitrified thereafter.	Diagnostic Test: Blood test Mesurement of E2, P4, LH, FSH hormones Diagnostic Test: Ultrasound Follicular measurement and endometrium measurement
Artificial (HRT) Cycles Start of estradiol valerate 4mg on day 2 of the cycle for three days. Increase E2 to 6mg on day 4 of E2 treatment. E2 dose may be increased according to clinician discretion based on endometrial thickness. Maximum time of E2 exposure will be 14 days. Transvaginally scan to monitor endometrial development and to exclude the presence of a dominant follicle. Serial measurements of serum LH, estradiol and progesterone levels. Commence the initial progesterone dose of 100mg at 22hrs (vaginal suppository) after ≥ 7 days and ≤ 16 days of estradiol administration when the minimal endometrial thickness achieved is 6mm with a trilaminar appearance. Subsequently increase progesterone administration to 100mg vaginally three times daily. Continue estradiol administration 6mg (3 tablets daily). Blastocyst transfer is scheduled on the 5th full day of progesterone administration, following the initial initiation of progesterone.	Diagnostic Test: Blood test Mesurement of E2, P4, LH, FSH hormones Diagnostic Test: Ultrasound Follicular measurement and endometrium measurement
Spontaneous natural cycles Ultrasound scans to monitor follicular growth and serial measurements of serum LH, estradiol and progesterone levels to determine the timing of ovulation. The LH surge will be considered to have begun when the concentration rises by 180% above the most recent serum value and continues to rise thereafter. Day 1 after the LH rise, a decrease in estradiol concentration is identified. Twenty four hours later progesterone concentrations rise with a level of greater than or equal to 1.5ng/ml confirming ovulation (day 0). This is considered as day 0 with initiation of vaginal progesterone 100mg (vaginal suppository) at 2200H. The following day (day 1) increases progesterone administration to 100mg vaginally three times daily (8 hourly) and continues this regime until 7 weeks gestation as per clinic protocol. Embryo transfer is scheduled 5 days (day 5) following confirmation of ovulation (day 0).	Diagnostic Test: Blood test Mesurement of E2, P4, LH, FSH hormones Diagnostic Test: Ultrasound Follicular measurement and endometrium measurement

Arm

Intervention/Treatment

Stimulated cycles

Ovarian stimulation will be performed by standard protocols. Stimulation medication dosage will be individualised prior to stimulation start according to the ovarian reserve parameters and during ovarian stimulation according to the ovarian response and the measured levels of E2 and progesterone (P4), in order to avoid progesterone elevation during late follicular phase. Final oocyte maturation will be achieved by administration of either 10.000 IU of hCG, 0.3 mg of GnRH agonist (Triptorelin) or dual trigger (hCG and GnRH-analogue), as soon as ≥ 3 follicles ≥ 17 mm are present. Oocyte retrieval will be carried out 36 hours after administration of the trigger. Embryos will undergo PGT-A at blastocyst stage and be vitrified thereafter.

Diagnostic Test: Blood test

Mesurement of E2, P4, LH, FSH hormones

Diagnostic Test: Ultrasound

Follicular measurement and endometrium measurement

Artificial (HRT) Cycles

Start of estradiol valerate 4mg on day 2 of the cycle for three days. Increase E2 to 6mg on day 4 of E2 treatment. E2 dose may be increased according to clinician discretion based on endometrial thickness. Maximum time of E2 exposure will be 14 days. Transvaginally scan to monitor endometrial development and to exclude the presence of a dominant follicle. Serial measurements of serum LH, estradiol and progesterone levels. Commence the initial progesterone dose of 100mg at 22hrs (vaginal suppository) after ≥ 7 days and ≤ 16 days of estradiol administration when the minimal endometrial thickness achieved is 6mm with a trilaminar appearance. Subsequently increase progesterone administration to 100mg vaginally three times daily. Continue estradiol administration 6mg (3 tablets daily). Blastocyst transfer is scheduled on the 5th full day of progesterone administration, following the initial initiation of progesterone.

Diagnostic Test: Blood test

Mesurement of E2, P4, LH, FSH hormones

Diagnostic Test: Ultrasound

Follicular measurement and endometrium measurement

Spontaneous natural cycles

Ultrasound scans to monitor follicular growth and serial measurements of serum LH, estradiol and progesterone levels to determine the timing of ovulation. The LH surge will be considered to have begun when the concentration rises by 180% above the most recent serum value and continues to rise thereafter. Day 1 after the LH rise, a decrease in estradiol concentration is identified. Twenty four hours later progesterone concentrations rise with a level of greater than or equal to 1.5ng/ml confirming ovulation (day 0). This is considered as day 0 with initiation of vaginal progesterone 100mg (vaginal suppository) at 2200H. The following day (day 1) increases progesterone administration to 100mg vaginally three times daily (8 hourly) and continues this regime until 7 weeks gestation as per clinic protocol. Embryo transfer is scheduled 5 days (day 5) following confirmation of ovulation (day 0).

Diagnostic Test: Blood test

Mesurement of E2, P4, LH, FSH hormones

Diagnostic Test: Ultrasound

Follicular measurement and endometrium measurement

Outcome Measures

Primary Outcome Measures

Ongoing pregnancy rate [12 weeks]
Ongoing pregnancy rate (≥ 12 weeks) in patients with endometrial compaction compared to patients without endometrial compaction after frozen embryo transfer of 1 or 2 euploid blastocysts

Secondary Outcome Measures

Biochemical pregnancy rate in HRT cycle [5 weeks]
Positive hCG, but at 5 gestational weeks no ultrasonographic visible gestational sac seen after embryo transfer in HRT-FET cycles with one or two euploid embryos, depending on the degree of compaction.
Biochemical pregnancy rate in spontaneous cycle [5 weeks]
positive hCG, but at 5 gestational weeks no ultrasonographic visible gestational sac seen) after embryo transfer in NC-FET cycles with one or two euploid embryos, depending on the degree of compaction.
Clinical implantation rate in HRT cycle [6 weeks]
Number of gestational sacs observed by ultrasound at 6 weeks of gestation divided by the number of embryos transferred), defined by a ß-hCG of > 5 IU on day 12 after embryo transfer in HRT-FET cycles with one or two euploid embryos, depending on the degree of compaction
Clinical implantation rate in spontaneous cycle [6 weeks]
Number of gestational sacs observed by ultrasound at 6 weeks of gestation divided by the number of embryos transferred), defined by a ß-hCG of > 5 IU on day 12 after embryo transfer in NC-FET cycles with one or two euploid embryos, depending on the degree of compaction.

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 40 Years

Sexes Eligible for Study:

Female

Inclusion Criteria:

Women aged 18 years to 40 years with regular menses (26-34 days)
Having 1 or 2 chromosomally normal cryopreserved blastocysts available for transfer after IVF / ICSI treatment
First frozen-thawed transfer cycle
Progesterone level < 1.5 ng/mL day of trigger injection in stimulation cycle from which embryos to be transferred were created.

Exclusion Criteria:

Polycystic ovarian syndrome
Poor ovarian responder in accordance with Bologna criteria
Uterine abnormality US / saline infusion sonohysterogram
Previous dilatation & curettage (D&C)
Hydrosalpinx
Asherman syndrome
History of endometriosis AFS ≥ 2
ICSI due to severe male factor with testicular sperm
Any known contraindications or allergy to oral estradiol or progesterone.
Discontinuation of HRT medication ( medication error in research HRT cycle )
Failure to detect ovulation in the research natural cycle
Ovulation after day 20 in a natural cycle
Duration of estradiol exposure ≥ 17 days and endometrium < 6mm
Spontaneous ovulation in HRT artificial cycle

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	IVI Middle East Fertility Clinic	Abu Dhabi		United Arab Emirates	60202

Sponsors and Collaborators

ART Fertility Clinics LLC

Investigators

Principal Investigator: Barbara Lawrenz, PhD, IVI Middle East Fertility Clinic LLC

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Barbara Lawrenz, Scientific Director, ART Fertility Clinics LLC

ClinicalTrials.gov Identifier:

NCT04454749

Other Study ID Numbers:

2003-ABU-002-BL

First Posted:

Jul 1, 2020

Last Update Posted:

Mar 8, 2021

Last Verified:

Mar 1, 2021

Individual Participant Data (IPD) Sharing Statement:

Undecided

Plan to Share IPD:

Undecided

Studies a U.S. FDA-regulated Drug Product:

Studies a U.S. FDA-regulated Device Product:

Keywords provided by Barbara Lawrenz, Scientific Director, ART Fertility Clinics LLC

Additional relevant MeSH terms:

Infertility

Infertility, Female

Study Results

No Results Posted as of Mar 8, 2021