Uterine Hemorrhage Clinical Trial
Official title:
Self-Administered Vaginal Misoprostol at Home for Cervical Ripening Prior to Outpatient Hysteroscopy: a Randomised Placebo-Controlled Trial.
To investigate if self-inserted vaginal misoprostol prior to outpatient hysteroscopy will lead to satisfactory cervical ripening, compared to placebo.
In gynaecological practice, diagnostic and therapeutic hysteroscopy is one of the most
common methods for diagnosing intrauterine pathology. The complications encountered during
hysteroscopy, such as cervical tears, creation of false passages, and uterine perforation,
are mainly related to the difficulty of cervical dilatation in nulliparous and
postmenopausal patients. GnRH agonist use, previous cone biopsy, and markedly retroverted
uterus are additional risk factors for complications.
Cervical ripening may be achieved either by mechanical means, such as with osmotic dilators,
or biochemically with prostaglandins. Solid evidence supports the efficacy of misoprostol
for cervical ripening before first-trimester suction curettage abortion. A consensus has
emerged that the optimal treatment regimen to use is 400-μg misoprostol 3-4 hours
pre-operatively, with vaginal administration being superior to the oral administration.
However, two studies using 400-μg misoprostol via the oral and vaginal routes have
previously shown that this does not result in satisfactory pre-operative dilatation in the
majority of Norwegian women, and we have recommended that the minimum dosage be greater than
400-μg vaginal misoprostol fours hours pre-operatively.
The first trials describing prostaglandin priming of the cervix to reduce the frequency of
traumatic cervical and uterine lesions in non-pregnant women prior to hysteroscopy were
published in 1985.
Misoprostol for cervical priming in non-pregnant women is not well established. 16 published
randomised controlled trials have shown different cervical response and outcomes. Most of
the studies have separately, but not systematically compared the effect on different patient
groups, such as nulliparous women and postmenopausal women. Seven of the studies included
less than 50 patients, and almost all the trials were underpowered as regards to evaluating
primary outcome measures. In the study with the largest number of patients included (Thomas
et al), the authors have not explained why or how they converted the primary outcome measure
from "the largest-number Hegar dilator that could be inserted without resistance" to a
binary variable ("Hegar > 8/Hegar < 8) after they had analysed their results - an apparent
protocol violation. It appears that none of the trials have been designed and conducted in
accordance with the CONSORT statement. The dosages used in the studies have varied between
200 and 1000-μg misoprostol given between 2 and 24 hours before hysteroscopy, via the oral,
sublingual and vaginal routes. Trials that have used higher dosages of misoprostol, via the
vaginal route, using the longest interval between administration of misoprostol and
hysteroscopy have tended to show more favourable outcomes as regards to cervical priming.
The hospital pharmacist will manufacture both active misoprostol ground up as a whitish
powder in capsules (500-μg per capsule), as well as an inactive ingredient with an identical
appearance (lactose) in capsules as placebo. The hospital pharmacist will prepare numbered,
opaque, sealed envelopes. The envelopes will be numbered according to a randomisation list.
The hospital pharmacy will then insert the prepared capsules into the envelopes. Each
envelope will contain two capsules. Half of the envelopes will contain two capsules with
500-μg misoprostol each, while the other half will contain two placebo capsules.
All patients referred to outpatient hysteroscopy at Ullevål University hospital will be sent
an invitation to be included in the study, together with dates for a prior out patient
consultation and the hysteroscopy. The study invitation will include detailed information
regarding the study, as well as an informed consent form. The out patient consultation will
take place a few days prior to their scheduled hysteroscopy, where they will be given the
option to participate in the study. The study authors will primarily be responsible for
recruiting patients. During the study period, participant flow will be recorded.
If the patients are recruited, the gynaecologist at the pre-operative consultation will
record the pre-operative variables on the case report form, and the patients will be given
an envelope containing the capsules before leaving the hospital. Hence those involved in
administering the intervention and assessing the outcomes will be blinded to the dosage, as
well as the patients. Each participant will be randomised by opening a numbered, sealed,
opaque envelope at home, containing either misoprostol, or an inactive ingredient with an
identical appearance, in capsules. The design method of randomization and blinding should
obviate potential subjectivity bias. The patients will be instructed to insert the capsules
at 9 p.m. the evening before the operation.
Before the hysteroscopy, the gynaecologist will measure the pre-operative degree of cervical
dilatation by passing Hegar dilators through the cervix in ascending order starting with a
size two millimetres. The size of the largest dilator passed into the cervical os without
subjective resistance felt by the operator will be recorded as the preoperative degree of
dilatation. If there is resistance with Hegar dilator size two millimetres, the result will
be recorded as < 2. Adverse events such as superficial cervical lacerations, false passage
of the cervix during cervical dilatation, and perforation of the uterus will be recorded.
The patient records will be reviewed after 60 days to see if the women have contacted the
hospital for post-operative complications.
A two sample sequential Wilcoxon test will be used to analyze the data. We performed a small
pilot study in our department on 20 patients prior to hysteroscopy in January 2006 to
investigate the pre-operative variability (SD) in cervical dilatation. The standard
deviation was 1.3 mm in postmenopausal patients (n=5), and 1.4 mm in premenopausal patients
(n=15). The mean cervical dilatation was 3.4 mm in postmenopausal patients and 5.4 mm in
premenopausal patients. The design of the main trial is based on a significance level of 5%
and a power of 95% against a 1 mm difference in the cervical dilatation caused by
misoprostol and placebo. As it seems unlikely that use of misoprostol could cause a
constriction of the cervix, a one-sided test is chosen. The trial will continue until either
the null hypothesis or the alternative hypothesis has been refuted.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
Status | Clinical Trial | Phase | |
---|---|---|---|
Completed |
NCT01968135 -
Does Concomitant Use of Combined Oral Hormonal Steroids Stop Bleeding in Women Using Etonogestrel Implants (Implanon/Nexplanon®)?: A Randomized Controlled Study
|
Phase 2 | |
Completed |
NCT04394234 -
A Study of Severe Uterine Bleeding Following Exposure to Direct Oral Anticoagulants
|
||
Completed |
NCT02147197 -
A Study of the Efficacy and Safety of a 3-month Treatment Course of Ulipristal Acetate for the Treatment of Abnormal Uterine Bleeding Associated With Leiomyomas
|
Phase 3 | |
Completed |
NCT01295294 -
Management of Initial Bleeding/Spotting Associated With the Levonorgestrel-releasing Intrauterine System (MIRENA)
|
Phase 4 | |
Recruiting |
NCT04867109 -
HE4 in the Diagnostic Approach of Endometrial Cancer in Patients With Postmenopausal Bleeding
|
||
Completed |
NCT02147158 -
A Study of the Efficacy and Safety of Ulipristal Acetate Intermittent Treatment for Abnormal Uterine Bleeding Associated With Leiomyomas
|
Phase 3 | |
Completed |
NCT01254799 -
Doxycycline in Treatment of Bleeding With Depot Medroxyprogesterone Acetate (DMPA)
|
Phase 3 | |
Completed |
NCT01726478 -
Uterotonic Efficacy of Oxytocin 2.5 Versus 10 Units During Caesarean Section at Mulago Hospital
|
N/A | |
Completed |
NCT00350480 -
Treatment of Non-Gestational Acute Uterine Bleeding: A Randomized Trial
|
N/A | |
Not yet recruiting |
NCT02453568 -
Use of Tranexamic Acid for Prevention of Postpartum Hemorrhage and Routine Blood Loss in Obstetrics
|
Phase 3 |