Clinical Trial Details
— Status: Active, not recruiting
Administrative data
| NCT number |
NCT04291001 |
| Other study ID # |
129999 |
| Secondary ID |
|
| Status |
Active, not recruiting |
| Phase |
Early Phase 1
|
| First received |
|
| Last updated |
|
| Start date |
September 4, 2020 |
| Est. completion date |
February 1, 2024 |
Study information
| Verified date |
November 2023 |
| Source |
University of Utah |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Same day initiation of the etonogestrel (ENG) implant and oral ulipristal acetate (UPA) would
overcome contraceptive access barriers to women with recent unprotected intercourse to
ongoing contraception. Current clinical guidelines recommend delaying implant initiation for
at least 1 week following UPA, as well as waiting 7 days before relying on the implant for
contraception after initiation alone. This pilot will assess the effects of the implant alone
and the implant inserted with same-day as UPA usage on ovarian activity. A total of 40 women
desiring the implant, who are not at risk for pregnancy during the study timeline, will be
recruited. Participants will be randomized to implant alone or same-day implant + oral UPA.
Participants will have daily ultrasounds and blood draws to assess timing of ovulation for 1
week and then an exit visit at 14 days after randomization. The primary outcome is the
incidence of ovulation in the 2 randomized treatment groups. Participants may continue the
implant after the study per FDA guidelines and rely on it for contraception after the study
is completed.
Description:
Primary Objectives:
1. To determine point estimates for the incidence of ovulation within five days of oral
ulipristal acetate (UPA) administration with same day etonogestrel (ENG) implant
insertion in the presence of a dominant follicle.
2. To determine point estimates for the incidence of ovulation within five days of
etonogestrel (ENG) implant insertion alone in the presence of a dominant follicle.
Secondary:
- Define the timing of ovulation in the 1st seven days following UPA with same day ENG
implant insertion in the presence of a dominant follicle.
- Define the timing of ovulation in the 1st seven days following ENG implant insertion in
the presence of a dominant follicle.
- Assess ovarian quiescence by ultrasound, Luteinizing hormone (LH) and progesterone
measurements 14 days (+/- 2 days) after implant initiation.
Clinical hypotheses:
- Combined oral UPA administration with same day ENG implant insertion will interfere with
UPA's effect in delaying ovulation as occurs with oral progestogens given within 1-2
days of UPA.
- The ENG implant alone delays ovulation beyond 5 days when initiated at the time of a
dominant follicle.
Study Design: Pilot randomized, single site clinical trial with blinded analysis
Participant recruitment and study site: The investigators will recruit participants
interested in using the ENG contraceptive implant but not currently at risk for pregnancy
from Planned Parenthood Association of Utah clinics, University of Utah Hospital and
Community clinics, and through targeted social media ads. All study procedures will occur at
the University of Utah Hospital Outpatient OBGYN Clinic or at the University Center for
Reproductive Medicine clinic.
Sample size: This is a pilot proposal to recruit a total of 40 participants across 2 study
arms: (1) ENG implant only (n=20) and (2) UPA + same day ENG implant insertion (n=20). The
investigators null hypotheses are:
1. ENG implant along with UPA administration in the presence of a dominant ovarian follicle
will not change the expected 97% ovulation suppression within 5 days of UPA use.
2. ENG implant insertion alone in the presence of a dominant ovarian follicle will not
sufficiently interrupt ovulation.
Randomization scheme: block randomization with block size of 4
Blinding protocol: This study will not be blinded as a pilot. The feasibility of the study,
including clinic space limitations and provider time, relies on the same healthcare provider
for implant insertion and ultrasound in many patients. All statistical analyses will be
blinded to the statistician.
Participant procedures:
Screening Visit (Screening Visit 1): Subjects will be screened for eligibility and interest
in the study. Each subject will have the study explained and, if participation is desired,
informed consent documents will be signed prior to any study procedures. The screening visit
will include: review of medical, surgical and social history, medications, menstrual dating,
sexual history and contraceptive use, physical exam, including breast and pelvic, pregnancy
test and a transvaginal ultrasound to ensure ability to document ovarian follicular activity
in the treatment cycle.
Progesterone Visit (Screening Visit 2): This brief visit will occur on days 20-24 of the
menstrual cycle and may be combined with the screening visit (Visit 1) if the time-frame is
met. This visit will include a review of any interim changes (if completed separate from the
screening visit) in history, medications, pregnancy risk/contraception, and a serum
progesterone level will be drawn. The participants will notify the study coordinator of the
1st day of their next menses.
Ovarian monitoring (Screening Visits 3-7 +/- 2 visits): Participants will undergo
transvaginal ultrasound evaluation of their ovaries three times a week starting on cycle day
#7 (+/- 2 days). If/ When investigators identify a lead follicle with a mean diameter of
>13mm in at least 2 dimensions, study follow-up will switch to daily monitoring.
Treatment Day #1 (Treatment Visit #1): Once a lead follicle (>14mm) is identified then
participants will be randomized to one of two treatment groups:
1. ENG implant insertion
2. UPA 30mg PO tablet and same-day ENG implant insertion Assigned treatment will be
administered (UPA and/or ENG implant insertion). Study team will obtain serum
progesterone, LH levels, and estradiol levels.
Treatment Days #2-8 (Treatment Visits #2-8): Participants will follow up daily for Days 2-8.
Each day investigators will obtain transvaginal ultrasound measurement of ovarian follicle
size, serum progesterone, LH levels, and estradiol levels. Daily transvaginal ultrasounds
will continue until either follicle rupture is documented, the follicle is <12 mm on two
consecutive visits, or Day 8 ultrasound occurs (7 days after implant insertion), whichever
occurs first.
Treatment Day #14 (Exit Visit): Repeat ultrasound will occur on Day 14 following ENG implant
insertion, and this will be the exit visit.
Data collection: Source documents for each participant and visit number will be completed by
the study personnel at the time of the visit. Form development, data collection, and data
management will occur in RedCAP, secure web platform for building and managing online
databases and surveys. Source documents maintained in individual participant binders.
Assessing and reporting adverse events: The reporting period for AEs is the period
immediately following the subject signing the informed consent through the 30 days following
the final study visit. Each visit will include assessment of how the participant felt since
the last visit, review of adverse event reports, implant insertion site reactions, lab
results, and vital signs and physical exam findings. AEs will not be reported for screen
failures unless a SAE is experienced during screening. For all AEs, the investigator will
pursue and obtain information adequate to determine the outcome of the AE and to assess
whether it met criteria for a SAE. Participants who have ongoing AEs or SAEs will be followed
until resolution or stabilization or referred for additional care. AEs will be documented
both on source documents and in the clinical database with SAEs reported per IRB guidelines.
Participants will be provided instructions for contacting the study site to report any
untoward medical occurrences. With permission from the participant, whenever possible records
from all non-study medical providers related to medical occurrences will be obtained for
review. AEs and SAEs will be reviewed by the Data Safety Monitoring Board.
Statistical Analyses:
The investigator and study team will be responsible for analyzing the study data. The
official clinical database in RedCAP will not be analyzed until medical/scientific review has
been completed, protocol violators have been identified (if appropriate), and data has been
declared complete.
Variables/Time Points of Interest The primary outcome is delay in rupture of the dominant
follicle by 5 days (yes/no) between group 1 (ENG implant alone) and group 2 (UPA with same
day ENG implant). If the date of follicle rupture was unclear by ultrasound
alone,investigators will utilize serum hormone levels to adjudicate day of rupture. These
measures include day of follicle collapse, day and value of highest LH, day and value of
highest progesterone level. Investigators will use an estradiol level of >100pg/ml to confirm
the enlarged follicle is the dominant follicle on the treatment day.
Statistical Methods The primary and secondary dichotomous outcome measures of ovulation by 5
days will be assessed by Wilcoxon sign rank test and demographic will be analyzed using
descriptive statistics.
Power/Sample Size:
The investigator and study team will be responsible for analyzing the study data. The
official clinical database in RedCAP will not be analyzed until medical/scientific review has
been completed, protocol violators have been identified (if appropriate), and data has been
declared complete.
Variables/Time Points of Interest The primary outcome is delay in rupture of the dominant
follicle by 5 days (yes/no) between group 1 (ENG implant alone) and group 2 (UPA with same
day ENG implant). If the date of follicle rupture was unclear by ultrasound alone,
investigators will utilize serum hormone levels to adjudicate day of rupture. These measures
include day of follicle collapse, day and value of highest LH, day and value of highest
progesterone level. Investigators will use an estradiol level of >100pg/ml to confirm the
enlarged follicle is the dominant follicle on the treatment day.
This is a pilot study to obtain point estimates for future study proposals. Current data on
ovulatory function with mid-cycle implant insertion or the pharmacodynamics interactions
between same day UPA and ENG are lacking.
Should data show that ovulation occurs <15% within 5 days of combined UPA use and ENG implant
initiation, investigators will pursue an adequately powered study assessing ovulation delay
with UPA only vs. UPA with ENG implant initiation. This finding would show that UPA's
relationship with the ENG implant may be different than what has been found with oral
progestogens. If ovulation occurs 15% in the first 5 days with combined use of these
medications, this would support the current practice of delaying implant insertion after UPA
administration.
Should data show that the ENG implant insertion alone in the presence of a dominant follicle
delays or stops ovulation >85%, investigators will pursue an adequately powered study
assessing the ENG implant alone for EC. If ovulation occurs >15%, this would support
continuation of the practice of using a backup method when an implant is inserted after the
first 7 days of the menstrual cycle.
These pre-specified criteria to judge if and how to proceed are consistent with CONSORT
guidelines for randomized pilot and feasibility trials.[11]
