Department of Obstetrics & Gynaecology, Royal Hospital, Muscat, Oman
*Corresponding Author e-mail: nooralqabas@hotmail.com

دراسة فاعلية ميسوبروستول كعالج غري جراحي حلاالت اإلجهاض يف الثلث
األول من احلمل

خربة املستشفى السلطاين، عمان

قمرية اأمبو�سعيدية و اأنيتا زت�سي

abstract: Objectives: Non-invasive methods of inducing a miscarriage are now considered an effective alternative
to surgical evacuation (dilatation and curettage). This study aimed to evaluate the effectiveness of misoprostol in the
termination of first-trimester miscarriages. Methods: This prospective study was conducted between October 2009
and September 2010 and assessed all patients admitted to the Royal Hospital in Muscat, Oman, for the termination
of first-trimester miscarriages during the study period. All patients received misoprostol and the rates of successful
termination were measured. Patient satisfaction was assessed using a short questionnaire. Results: A total of 290
women were included in the study. Termination with misoprostol was successful in 61.38% of the subjects. Of the
remaining subjects requiring additional surgical evacuation (n = 112), 58.93% required evacuation due to failed
termination with misoprostol and 65.18% underwent early evacuation (≤24 hours since their last misoprostol dose).
The majority of patients experienced no side-effects due to misoprostol (89.66%). Pain was controlled with simple
analgesics in 70.00% of the subjects. A high satisfaction rate (94.83%) with the misoprostol treatment was reported.
Conclusion: Misoprostol was a well-tolerated drug which reduced the rate of surgical evacuation among the study
subjects. This medication can therefore be used safely in the management of incomplete miscarriages.

Keywords: Misoprostol; First Trimester Pregnancy; Miscarriage; Incomplete Abortion; Dilation and Curettage;
Oman.

امللخ�ص: الهدف: تعترب العالجات غري اجلراحية حلث الإجها�ض˗يف الوقت احلايل˗فعالة و بدائل ماأمونة للتفريغ اجلراحي. هدفت هذه
ا�ستطالعية )م�ستقبلية( درا�سة احلمل. الطريقة: من الأول الثلث يف احلمل˗الإجها�ض لإنهاء املي�سوبرو�ستول فاعليةعقار لتقييم الدرا�سة
يف الفرتة ما بني اأكتوبر 2009 و �سبتمرب 2010. �سمت الدرا�سة جميع املري�سات اللواتي مت قبولهن يف ق�سم اأمرا�ض الن�ساء يف امل�ست�سفى
ال�سلطاين˗م�سقط، �سلطنة عمان˗لإنهاء الإجها�ض يف الثلث الأول من احلمل با�ستخدام اأقرا�ض املي�سوبرو�ستول. مت قيا�ض فاعلية العالج
املي�سوبرو�ستول عقار جنح الدرا�سة. يف مري�سة 290 �ساركت النتائج: ق�سري. با�ستبيان للعالج املري�سات قبول م�ستوى تقييم مت كما
ب�سبب منهن 58.93% اجلراحي، التفريغ لعملية حالة 112 خ�سعت الدرا�سة. يف امل�ساركات من 61.38% يف الإجها�ض اإحداث يف كان
ف�سل املي�سوبرو�ستول. وقد لوحظ اأن التفريغ اجلراحي قد مت خالل فرتة اأق�رس من 24 �ساعة من اأخذ اأقرا�ض املي�سوبرو�ستول يف 65.18%
من احلالت. مل تكن هناك اأي م�ساعفات يف %89.66 من احلالت. مت ت�سكني الأمل ل %70.00 من احلالت مب�سكنات ب�سيطة. تقبلت معظم
املري�سات العالج ب�سكل جيد. اخلال�صة: املي�سوبرو�ستول هو دواء جيد وي�ساعد على تقليل معدل عمليات التفريغ اجلراحي و ميكن ا�ستخدامه

باأمان لعالج حالت الإجها�ض غري املكتمل.
مفتاح الكلمات: املي�سوبرو�ستول؛ الثلث الأول من احلمل؛ اإجهَا�ض؛ اإجها�ض غري مكتمل؛ تفريغ جراحي للرحم؛ عمان.

Effectiveness of Misoprostol for Induction of
First-Trimester Miscarriages

Experience at a single tertiary care centre in Oman
*Qamariya Ambusaidi and Anita Zutshi

Advances in Knowledge
- This study is the first in Oman to investigate the effectiveness of misoprostol in inducing first-trimester miscarriages.
- Results from this study showed that the medication had minimal side-effects among the studied group of women.

Application to Patient Care
- Surgical evacuations can result in complications that affect future obstetric outcomes, including cervical incompetence, uterine

perforation, intrauterine adhesions and morbidly adherent placenta. Misoprostol is a non-invasive alternative to induce miscarriage
and avoid these potential complications.

- Misoprostol is currently not available in all hospitals in Oman. The results of this study may help to encourage wider utilisation of this
medication in inducing miscarriages.

clinical & basic research

Sultan Qaboos University Med J, November 2015, Vol. 15, Iss. 4, pp. e534–538, Epub. 23 Nov 15
Submitted 4 Feb 15
Revision Req. 10 May 15; Revision Recd. 17 May 15
Accepted 18 Jun 15 doi: 10.18295/squmj.2015.15.04.016

Qamariya Ambusaidi and Anita Zutshi

Clinical and Basic Research | e535

Miscarriage is defined as a pregnancy that ends spontaneously before the fetus is viable. The most common complication
of early pregnancy is miscarriage; Robledo et al.
estimated that approximately 8–20% of clinically
recognised pregnancies under 20 gestational weeks
end in miscarriage, with 80% occurring in the first 12
gestational weeks.1 Three options exist for managing
a miscarriage in a patient: expectant management,
surgical evacuation or medical/pharmaceutical
management. While surgical evacuation is a fast and
effective procedure when performed by a well-trained
physician, it is nevertheless a blind and invasive
procedure that carries a risk of injury, bleeding and
infection, in addition to possible complications from
the anaesthesia. Medical methods for the induction of
miscarriage are now considered an effective alternative
to surgical evacuation. Prostaglandin analogues, of
which misoprostol is the most common, are widely
utilised in several countries. In 2009, 40%, 72% and
76% of abortions were induced via medication in the
UK, Sweden and Finland, respectively.2

Misoprostol is a synthetic prostaglandin E1
analogue which causes uterine contractions and
softening and dilation of the cervix. It has been used off-
label in the management of miscarriage, postpartum
haemorrhage, induction of labour and ripening of the
cervix.3 Although misoprostol is not yet licensed by
the Food and Drug Administration in the USA for the
above indications, pregnancy was removed from the
list of absolute contraindications to misoprostol use
in 2002.4 The advantages of misoprostol include its
low cost, long shelf life, lack of need for refrigeration
and worldwide availability.3 The aim of this study was
to evaluate the success of misoprostol as an agent for
medical termination in first-trimester miscarriages at
the Royal Hospital, Muscat, Oman.

Methods

This prospective study was conducted between
October 2009 and September 2010 and included
all patients admitted for the termination of a first-
trimester miscarriage to the Gynaecology Ward at the
Royal Hospital during the study period. The exclusion
criteria were termination of a viable pregnancy and
absolute contraindications for misoprostol, including
patients with a suspected or confirmed ectopic
pregnancy, gestational trophoblastic diseases, a high
risk of uterine rupture, an intrauterine device in
situ, an allergy to prostaglandins or haemodynamic
instability. Women who underwent a medical termi-
nation of pregnancy for maternal or fetal indications

were excluded from the study and only those with a
diagnosis of an incomplete or missed/silent miscarriage
were included. All subjects underwent a thorough
physical examination. Baseline characteristics, inclu-
ding age, parity, gestational age and type of mis-
carriage, were obtained. A complete blood count
was performed to assess pre-treatment haemoglobin
levels in all candidates, in addition to blood grouping.
Rhesus typing and antibody screening tests were
also performed.

All of the subjects were given misoprostol accor-
ding to hospital protocol. Patients with incomplete
miscarriages received a single oral dose of 600 µg of
misoprostol. Those with missed miscarriages received
vaginal misoprostol with a maximum of three doses
of 800 µg every 24 hours. Vaginal misoprostol was
avoided for patients with vaginal bleeding or leaking
and for those with a high white blood cell count. In
such cases, the same dose was given orally. For
patients with previous uterine scarring, a half dose
of misoprostol was given. All of the subjects were
admitted as inpatients to monitor bleeding and the
development of any side-effects. Patients’ analgaesia
requirements were also recorded. All patients
with Rhesus-negative blood were given an anti-D
immunoglobulin injection before discharge.

The complete miscarriage rate was determined
to assess the efficacy of misoprostol. Complete
miscarriages were defined as successful cases
that did not require surgical evacuation after the
administration of misoprostol. Ultrasonography was
performed on each patient to confirm that no products
of conception remained. Diagnosis of a complete
miscarriage was based on the clinical judgment of
the attending obstetrician. However, an endometrial
thickness of 14 mm was considered to be the cut-off
value for a complete miscarriage. Retained products
of conception indicated the need for a surgical
evacuation. The time interval between the last dose of
misoprostol and surgical evacuation was also assessed.
Following the completion of their treatment with
misoprostol, patient satisfaction was determined using
a short questionnaire. Responses to the following two
questions were recorded: “Are you satisfied with the
treatment?” and “If you have a similar problem in the
future, are you going to use misoprostol again?”.

Data were analysed using the Statistical Package for
the Social Sciences (SPSS), Version 17.0 (IBM Corp.,
Chicago, Illinois, USA). This study was approved by
the Medical Ethics & Scientific Research Committee
of the Royal Hospital (MESRC #37). All patients
gave informed verbal consent prior to their inclusion
in the study.

Effectiveness of Misoprostol for Induction of First-Trimester Miscarriages
Experience at the Royal Hospital, Oman

e536 | SQU Medical Journal, November 2015, Volume 15, Issue 4

Results

A total of 290 women with first-trimester miscarriages
were admitted to the Royal Hospital during the study
period. The mean age was 32.9 years and mean parity
was 2.6. The majority of the subjects were admitted
due to a diagnosis of incomplete miscarriage (63.45%).
Fetal age ranged from 5–12 gestational weeks with a
mean age of 9.4 gestational weeks. The overall rate of
complete termination with misoprostol was 61.38%,
while 38.62% of cases required further surgical
evacuation.

A total of 112 patients underwent surgical
evacuation. The indications for surgical evacuation
are shown in Figure 1. The vast majority of patients
discontinued misoprostol and underwent evacuation
because of failed termination with the drug
(58.93%). The second most common indication was
bleeding (19.64%), although seven patients only had
postevacuation haemoglobin levels for comparison.
Four patients experienced a significant drop in
haemoglobin levels (>2.0 g/dL). However, only one
patient required a blood transfusion. The mean drop

in haemoglobin level was 2.2 g/dL [Figure 2]. Surgical
evacuation was carried out for 19 patients who refused
to continue the misoprostol treatment. Three patients
underwent a surgical evacuation due to fever and one
patient due to a suspected septic abortion indicated by
foul smelling discharge, although a subsequent culture
was negative for infection. The distribution of patients
undergoing surgical evacuation by miscarriage type is
shown in Figure 3.

Early surgical evacuations (within 24 hours of the
last dose of misoprostol) were performed for 65.18%
of the subjects. After excluding cases with bleeding
and suspected infection, 44.64% of the women
who underwent a surgical evacuation due to failed
termination did so within 24 hours of receiving their
last dose of misoprostol. Only 10.71% of the patients
underwent surgical evacuation after 72 hours [Figure 4].

The majority of patients experienced no side-effects
from misoprostol (89.66%). The remaining women
had the following side-effects: bleeding (7.59%), fever
(2.41%) and chills (0.34%). All patients with significant
bleeding based on the subjective assessment of the
attending doctor underwent surgical evacuation.
All of the febrile women had fevers which subsided

Figure 1: Indications leading to surgical evacuation
after the use of misoprostol among patients admitted
for the termination of first-trimester miscarriages
(N = 112).

Figure 3: Distribution of patients undergoing suction
evacuation according to their miscarriage diagnosis
among patients admitted for the termination of first-
trimester miscarriages (N = 112).

Figure 2: Haemoglobin levels pre- and post-treatment with
misoprostol among patients admitted for the termination
of first-trimester miscarriages and who underwent suction
evacuation for heavy vaginal bleeding (N = 7).
Hb = haemoglobin.

Figure 4: Time interval between the last dose of
misoprostol and surgical evacuation among patients
admitted for the termination of first-trimester
miscarriages and requiring evacuation (N = 112).

Qamariya Ambusaidi and Anita Zutshi

Clinical and Basic Research | e537

within 24 hours. None of the patients experienced
any gastrointestinal side-effects. Only one patient
experienced prolonged bleeding lasting for four weeks
after management with misoprostol; she underwent
a surgical evacuation and subsequent histopathology
showed only blood clots with no retained products of
conception.

Analgaesics were offered to all of the patients,
but the majority tolerated the pain well. Pain was
controlled with paracetamol and non-steroidal anti-
inflammatory drugs (NSAIDs) such as mefenamic
acid, diclofenac sodium tablets or intramuscular
injections in 70.00% of patients. Of the remaining
patients, 26.55% did not require analgesia, while 3.45%
received tramadol due to NSAID allergies.

In terms of patient satisfaction, 277 subjects (95.52%)
said they were satisfied with misoprostol. Of these, 275
indicated that they would use it again. Despite their
satisfaction, the remaining two patients stated that they
would not undergo misoprostol treatment a second
time due to the longer hospital stay required. Of the 13
patients who were not satisfied with misoprostol, two
nevertheless stated that they would try it again in the
future in order to avoid the potential complications of a
surgical evacuation [Table 1].

Discussion

During their reproductive years, 25.00% of all women
will experience at least one early pregnancy miscar-
riage.1 Suction evacuation is the usual treatment for
miscarriage, regardless of gestational age. In three
small randomised controlled trials, expectant manage-
ment showed a success rate of 79.00% in three days
for incomplete miscarriages and only 37.00% in seven
days for silent miscarriages.5 There were no differences
in complication rates.5

Studies have suggested that pregnancy termination
efficacy may be higher among early pregnancies (six
gestational weeks). Faúndes et al. determined that the
rate of effectiveness for misoprostol in first-trimester
pregnancy terminations was 85.00%.6 Davis et al. also

reported a success rate of 85.00% for misoprostol.7
However, they noted that post-treatment bleeding
occurred for longer periods of time with misoprostol,
although none of the patients required a blood
transfusion.7 The duration of post-treatment bleeding
was difficult to assess in the current study as most cases
were straightforward and were therefore followed-up
by local general practitioners outside of the Royal
Hospital. Chen et al. reported that nearly 30.00% of
deliveries in the USA were performed via Caesarean
section;8 it is therefore not surprising that many
women who suffer from miscarriages also have a
history of uterine surgery. Misoprostol may be a
preferable option for these patients. In the present
study, there were no cases of uterine rupture or
adverse outcomes.

Misoprostol can be administered at different doses
and through different routes (vaginal, oral, sublingual
or rectal). A Cochrane review of 19 randomised
controlled trials indicated that the vaginal route is
the best option, with no significant difference in side-
effects.9 Vaginal misoprostol administration results
in slower absorption of the drug and longer duration
of stimulation in comparison to oral administration.
The sublingual route avoids the first-pass effect and
is associated with more rapid absorption and higher
peak levels than those obtained with other routes.9
Misoprostol is usually administered vaginally in three
doses of 800 µg each; this regimen has been found to
yield a success rate of 90.00% in the first trimester,
with 80.00% and 95.00% of patients expelling the
products of conception within 24 and 48 hours of
the dose, respectively.5 The same treatment plan was
used in the current study but had lower success rates
due to early intervention with surgical evacuation.
It should be noted that the majority of patients who
underwent a surgical evacuation in the current study
did so within 48 hours of their last misoprostol dose.
The efficacy of misoprostol is related to the dosage as
a lower dose will have a weaker effect. However, the
rate of side-effects does not seem to be related to the
dosage. While sublingual misoprostol has a similar
efficacy to vaginal misoprostol, Gemzell-Danielsson
et al. observed that this route was associated with
more frequent side-effects (e.g. diarrhoea).10

Different factors may have influenced the
decision for surgical evacuation in the current study.
Importantly, misoprostol was restricted to inpatient
use only and there was pressure from both the patients
and hospital administration to shorten hospital stays,
increase patient turnover and reduced patient overflow
and bed shortages. Early interventions in first trimester
miscarriages could be minimised by the initiation of
misoprostol as an outpatient treatment. Additionally,

Table 1: Patient satisfaction with the use of misoprostol
among patients admitted for the termination of first-
trimester miscarriages (N = 290)

Willingness to try
treatment again in

future

Total

No Yes

Satisfaction
with treatment

No 11 2 13

Yes 2 275 277

Total 13 277 290

Effectiveness of Misoprostol for Induction of First-Trimester Miscarriages
Experience at the Royal Hospital, Oman

e538 | SQU Medical Journal, November 2015, Volume 15, Issue 4

delaying the assessment of misoprostol efficacy until
a week after the last dose is recommended. However,
more studies on this topic are needed.

Side-effects of misoprostol are usually transient
and self-limiting. The most commonly reported
side-effect is vaginal bleeding, which can last for
2–6 weeks. Faúndes et al. reported a mean drop
in haemoglobin levels of 0.2–1.0 g/dL for patients
receiving misoprostol, although blood transfusions
were rarely necessary.6 In the current study, the
mean drop in haemoglobin was significant, with one
patient requiring a blood transfusion. There is no clear
reason for this discrepancy; however, pre-existing
iron deficiencies and anaemia may have contributed
to the low haemoglobin levels detected. Abdominal
cramping beginning as early as 30 minutes after
administration of the drug is another common side-
effect of misoprostol.6 For this reason, most patients in
the present study were given analgesics and NSAIDs
concurrently with misoprostol.

There is no consensus regarding the use of
antibiotics during treatment of miscarriage. Although
research has shown that the infection rate is lower after
a medical/pharmaceutical induction of miscarriage,
it is important to note that antibiotics are more
commonly used after pharmaceutical inductions
rather than surgical evacuations.6 In this study, the
decision to use post-procedure antibiotics was left to
the treating physician.

Patient satisfaction is a useful measure to
determine the efficacy of any treatment and assess
the quality of healthcare provision. Additionally,
patient satisfaction rates indicate acceptance of a
treatment. In the present study, two direct close-ended
questions were used to assess satisfaction among the
subjects. However, general patient satisfaction was
not assessed beyond the acceptance of misoprostol
as an alternative to surgical evacuation. Ideally,
patients should be surveyed regarding a wide range
of factors associated with their treatment, including
inpatient care, experience with misoprostol, route of
misoprostol administration, type of analgesia received
and patient-provider relationship. The current study is
also limited as a more precise satisfaction rate could
have been determined by analysing women who had
had previous surgical evacuations and comparing
them with women receiving pharmaceutical treatment
for a current miscarriage.

Conclusion

Misoprostol was an effective treatment for the
management of first-trimester miscarriages in the
studied group. The administration of misoprostol

significantly reduced the surgical evacuation rate
with minimal side-effects. Subjects reported high
rates of satisfaction and acceptance with misoprostol.
Therefore, misoprostol is recommended as a safe
drug for use among outpatients with incomplete
miscarriages as an alternative to surgical evacuation.

c o n f l i c t o f i n t e r e s t
The authors declare no conflicts of interest.

References
1. Robledo C, Zhang J, Troendle J, Barnhart K, Creinin MD,

Westhoff C, et al. Clinical indictors for success of misoprostol
treatment after early pregnancy failure. Int J Gynaecol Obstet
2007; 99:46–51. doi: 10.1016/j.ijgo.2007.04.031.

2. Niinimäki M, Suhonen S, Mentula M, Hemminki E,
Heikinheimo O, Gissler M. Comparison of rates of adverse
events in adolescent and adult women undergoing medical
abortion: Population register based study. BMJ 2011; 342:d2111.
doi: 10.1136/bmj.d2111.

3. Allen R, O’Brien BM. Uses of misoprostol in obstetrics and
gynecology. Rev Obstet Gynecol 2009; 2:159–68. doi: 10.3909/
riog0055.

4. American College of Obstetrician and Gynecologists. ACOG
Committee Opinion: Number 283, May 2003 - New U.S. Food
and Drug Administration labeling on cytotec (misoprostol)
use and pregnancy. Obstet Gynecol 2003; 101:1049–50.
doi: 10.1016/S0029-7844(03)00396-X.

5. Trinder J, Brocklehurst P, Porter R, Read M, Vyas S, Smith L.
Management of miscarriage: Expectant, medical, or surgical?
Results of randomised controlled trial (miscarriage treatment
(MIST) trial). BMJ 2006; 332:1235–40. doi: 10.1136/
bmj.38828.593125.55.

6. Faúndes A, Fiala C, Tang OS, Velasco A. Misoprostol for
the termination of pregnancy up to 12 completed weeks
of pregnancy. Int J Gynaecol Obstet 2007; 99:S172–7.
doi: 10.1016/j.ijgo.2007.09.006.

7. Davis AR, Hendlish SK, Westhoff C, Frederick MM, Zhang J,
Gilles JM, et al. Bleeding patterns after misoprostol vs surgical
treatment of early pregnancy failure: Results from a randomized
trial. Am J Obstet Gynecol 2007; 196:e1–7. doi: 10.1016/j.
ajog.2006.07.053.

8. Chen BA, Reeves MF, Creinin MD, Gilles JM, Barnhart K,
Westoff C, et al. Misoprostol for treatment of early pregnancy
failure in women with previous uterine surgery. Am J Obstet
Gynecol 2008; 198:e1–5. doi: 10.1016/j.ajog.2007.11.045.

9. Canadian Pharmacists Association. Compendium of Pharma-
ceuticals and Specialties: The Canadian drug reference for
health professionals. Ottawa, Canada: Canadian Pharmaceutical
Association, 2005.

10. Gemzell-Danielsson K, Ho PC, Gómez Ponce de León R,
Weeks A, Winikoff B. Misoprostol to treat missed abortion
in the first trimester. Int J Gynecol Obstet 2007; 99:S182–5.
doi: 10.1016/j.ijgo.2007.09.008.

http://dx.doi.org/10.1016/j.ijgo.2007.04.031
http://dx.doi.org/10.1136/bmj.d2111
http://dx.doi.org/10.3909/riog0055
http://dx.doi.org/10.3909/riog0055
http://dx.doi.org/10.1016/S0029-7844%2803%2900396-X
http://dx.doi.org/10.1136/bmj.38828.593125.55
http://dx.doi.org/10.1136/bmj.38828.593125.55
http://dx.doi.org/10.1016/j.ijgo.2007.09.006
http://dx.doi.org/10.1016/j.ajog.2006.07.053
http://dx.doi.org/10.1016/j.ajog.2006.07.053
http://dx.doi.org/10.1016/j.ajog.2007.11.045
http://dx.doi.org/10.1016/j.ijgo.2007.09.008