Endometrial Transcript Profile with Progesterone After Post-ovulatory Mifepristone

Determinaton of Changes in the Endometrial Gene Expression Profile Induced by Exogenous Progesterone After Post-ovulatory Administration of Mifepristone

Status

Completed

Phases

Early Phase 1

Study type

Interventional

Source

ClinicalTrials.gov

Registry ID

NCT06616077

Enrollment

Registered

2024-09-27

Start date

2022-06-07

Completion date

2023-05-08

Last updated

2024-09-27

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Endometrial Endocrine Regulation, Progesterone Supplementation in Women After Mifepristone

Keywords

Endometrial gene expression, Progesterone, Mifepristone, RU486, Secretory endometrium

Brief summary

The goal of this exploratory trial is to determine the endometrial gene expression profile induced by exogenous progesterone after postovulatory administration of mifepristone. It will also learn about the plasticity ofr the endometrial response to progesterone. The main questions it aims to answer are: Is exogenous progesterone able to modulate the gene expression of endometrial transcripts that have been altered by mifepristone? Researchers will compare the endometrial gene expression profiles with exogeonous progesterone to a placebo (a look-alike substance that contains no drug) after postovulatory administration of mifepristone. Participants will: Do ovulation follow-up tests at home assesing LH in urine Visit the hospital 2 days after a positive LH for mifepristone administration and ultrasonography check of ovaries and uterus. Starting from the next day, take progesterone or placebo for 3 days. Visit the hospital 2 days after that for ultrasonography check of ovaries and uterus and for an endometrial and blood sample collection. The endometrial samples will be processed to isolate the RNA and for histological assessment. Gene expression profiles will be determined by RNA-seq.

Detailed description

Objective: To determine the effect of progesterone supplementation on the mid-secretory endometrial transcript profile after postovulatory administration of mifepristone. Design: A randomized, double-blind, placebo-controlled study. Setting: Tertiary academic medical center Subjects: A total of 9 Hispanic women of proven fertility who had been surgically sterilized. Interventions: Participating women received a single dose of mifepristone 200mg 48 hours after the LH peak (LH+2, LH+0=LH peak). Endometrial samples were obtained on LH+7 after vaginal administration of micronized progesterone (600mg/day) for 3 days (LH+3 to LH+5). Each woman contributed with one cycle treated with placebo and another with progesterone (group A). Additionally, endometrial samples were obtained on LH+7 from subset of 4 women who did not receive mifepristone; with each one contributing with one cycle treated with vaginal progesterone supplementation or placebo as a reference (group B). Endometrial thickness, circulating progesterone levels, and endometrial histology were also documented in all cycles. RNA-seq was used to identify genes whose transcript levels significantly changed by the administration of progesterone versus placebo, with postovulatory administration of mifepristone. The transcript profiles of these genes were further evaluated in the endometrial samples from group B.

Interventions

DRUGMicronized Progesterone 600 mg

Vaginal supplementary micronized progesterone will be given after postovulatory administration of the progesterone receptor antagonist mifepristone. Administration from LH+3 to LH+5 (LH peak=LH+0); 200 mg 3 times per day.

DRUGmifepristone 200 mg

Post ovulatory single oral administration (LH+2, LH peak=LH+0)

DRUGOral Placebo Tablet

Oral placebo tablet containing brewer yeast, cellulose, stearic acid, silica, magnesium stearate

DRUGPlacebo Vaginal

Cocoa butter

Study design

Allocation

RANDOMIZED

Intervention model

CROSSOVER

Primary purpose

BASIC_SCIENCE

Masking

DOUBLE (Subject, Caregiver)

Eligibility

Sex/Gender

FEMALE

Age

18 Years to 43 Years

Healthy volunteers

Yes

Inclusion criteria

* proven fertility * regular menstrual cycles * surgically sterilized at least one year before participating in the protocol

Exclusion criteria

* chronic medical problems * abnormal results of screening blood tests * ovarian masses * symptomatic endometriosis * uterine leiomyomata * being under chronic medication or taking hormones or drugs able to modify the metabolism of steroid hormones in the 3 preceding months to study enrollment

Design outcomes

Primary

Measure	Time frame	Description
Endometrial Gene Expression Profile	From enrollment to the end of treatments after aproximately 12 weeks	RNA-seq gene expression in the midluteal phase

Secondary

Measure	Time frame	Description
Endometrial dating	From enrollment to the end of treatments after aproximately 8 months	Estimated cycle day based on endometrial morphology according to the Noyes criteria

Other

Measure	Time frame	Description
Uterine ultrasonographic features	From enrrollment to the end of treatments after 12 weeks	Will be evaluated the ultrasonographic features such as hypo- and hyper- echogenecity
Circulating progesterone levels	From enrollment to after the treatments after 12 weeks	Will be evaluated the cirduating levels of progesterone on day LH+7 (LH+0=LH peak) in women that have taken postovulatory mifepristone plus exogenous progesterone or placebo.

Countries

Chile

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026