Effect of Adjunctive Misoprostol Treatment on Blood Loss at Vaginal Delivery
| Status: | Completed |
|---|---|
| Conditions: | Women's Studies |
| Therapuetic Areas: | Reproductive |
| Healthy: | No |
| Age Range: | 18 - Any |
| Updated: | 3/16/2019 |
| Start Date: | March 30, 2012 |
| End Date: | February 16, 2019 |
Effect of Adjunctive Misoprostol on Blood Loss at Vaginal Delivery
This document defines the Clinical Investigation Protocol for a study designed to determine
whether blood loss after spontaneous vaginal delivery is altered by the addition of
misoprostol administration to the standard use of intravenous oxytocin after delivery. The
protocol is an open-label randomized prospective trial to be carried out at Queens Hospital
Center.
Blood loss will be measured indirectly by comparing the maternal hemoglobin and hematocrit
levels on admission in labor to those obtained within 24 hours after delivery.
whether blood loss after spontaneous vaginal delivery is altered by the addition of
misoprostol administration to the standard use of intravenous oxytocin after delivery. The
protocol is an open-label randomized prospective trial to be carried out at Queens Hospital
Center.
Blood loss will be measured indirectly by comparing the maternal hemoglobin and hematocrit
levels on admission in labor to those obtained within 24 hours after delivery.
Background Some maternal blood loss normally occurs at the time of vaginal delivery. The best
estimates indicate that a loss of approximately 500 mL is average, with a range of about
250-700 mL.[1,2] Some of this bleeding arises from birth canal lacerations or surgical
incisions (i.e., episiotomy), but most derives from the vessels exposed in the uterine wall
at the placental site once the placenta has separated.
Under normal circumstances, shortly after placental separation intense myometrial
contractions occur. These raise the pressure within the myometrial wall above that of the
blood pressure in the vessels that traverse it, vessels that opened into the intervillous
space. Flow in these vessels is thus mechanically attenuated by myometrial contraction,
allowing for the formation of intravascular thrombi.
This mechanism for controlling postpartum uterine blood loss works well most of the time. If,
however, the uterus remains hypotonic or atonic after delivery, excessive blood loss can
occur. In the worst cases, severe uterine hemorrhage ensues. Postpartum hemorrhage is, in
fact, the leading cause of maternal mortality in the world, accounting for at least 100,000
deaths annually.[3] Even in the absence of frank hemorrhage, postpartum blood loss can result
in maternal anemia. Recuperation of iron stores to recover from this blood loss takes time,
and may not occur, especially in low socioeconomic areas where dietary iron consumption is
often deficient, and pregnancies tend to occur in close succession.
Postpartum anemia is a significant contributor to short- and long-term morbidity.[5-7] It
increases the risk of infection and poor wound healing. Also, the associated fatigue may
interfere with the mother's ability to administer child care and to bond appropriately with
her infant. Anemic mothers tend to have more difficulty with nursing, and may produce
iron-deficient milk. There is thus a strong rationale to minimize postpartum blood loss.
In most US hospitals, parturients receive a high dose of intravenous or intramuscular
oxytocin immediately after delivery. This approach has been shown in several studies to
reduce the risk of postpartum hemorrhage, [8-11] and is practiced routinely at Queens
Hospital Center. Investigators will employ an intravenous infusion of oxytocin (Pitocin®) at
a rate of about 50-100 mU/minute. Despite this approach, there is still substantial blood
loss at delivery, based on the investigator's preliminary observations shown below. This
provides the rationale to determine whether use of an adjunctive drug, namely misoprostol 600
µg rectally, administered after delivery, might reduce blood loss further than does oxytocin
alone, thus decreasing the risk of morbidity related to postpartum anemia.
Preliminary Data
The investigators examined the hemograms of a randomly chosen consecutive sample of 53
spontaneous vaginal deliveries performed at Queens Hospital Center between September 15 and
October 1, 2010.
Among these patients, the admission hemoglobin concentration was 11.9±1.2 g/dL and that on
the first postparutum day was 10.9±1.3. The mean fall was 1.02 (95% CI 0.74, 1.29), a
statistically significant decrease (P<0.0001). Hematocrit levels fell in parallel, by an
average of 7.8% of the predelivery value. The mean fall in hemoglobin and hematocrit levels
after delivery (1.02 g/dL and 2.81%) is consistent with an average blood loss of about 500
mL. The consistency of these changes and the small associated variance indicate that the
change in hemoglobin and hematocrit levels is a meaningful proxy for the assessment of blood
lost during vaginal delivery.
Study Design The study is a prospective randomized open-label clinical trial to be performed
in a single institution. It will compare the intrapartum and postpartum maternal blood
hemoglobin concentrations and hematocrit measurements in a group of parturients who received
standard prophylactic intravenous oxytocin immediately after delivery with a group that
received oxytocin and adjuvant misoprostol.
Sample size and analysis
A total of 800 subjects will enter this two-treatment parallel design study. With that sample
size, the probability is 90% that the study will detect a treatment difference at a two-sided
0.05 significance level if the difference in hemoglobin concentration between treatments is
0.3 g/dL. This analysis is based on the assumption that the standard deviation of the
postpartum and intrapartum hemoglobin concentrations is not larger than 1.3 g/dL.
Comparison of intrapartum and postpartum hemoglobin and hematocrit levels will be done using
a paired t-test. A probability level of 0.05 will be used as the threshold for significance.
Inclusion and exclusion criteria This study will include adult pregnant women regardless of
age. Pregnant minors under the age of 18 will not be eligible.
A patient will be considered for inclusion in the study if she meets all of the following
criteria:
- She has a term (≥37 completed weeks) live singleton gestation in cephalic presentation
and has been admitted to the Labor and Delivery Unit
- She is in the latent phase of labor or has been admitted for induction of labor or at
prenatal clinic visit
- She has had fewer than four prior vaginal deliveries.
- She reports no allergy to misoprostol.
The following factors or conditions will exclude a patient from consideration as a subject:
- The fetus has a known major fetal malformation or chromosome abnormality
- The gestation is multiple.
- There is a breech or other malpresentation
- The patient reports involvement in another clinical trial currently or previously in
this pregnancy.
- The patient is expected to have a cesarean delivery.
- The patient had a prior cesarean delivery.
- There has been an intrauterine fetal death.
- There is polyhydramnios (amniotic fluid index >22 cm).
- Presence of acute or chronic renal disease
- Presence of preeclampsia
Of subjects who enter the study, the development of certain conditions will exclude them post
hoc from receiving misoprostol under the protocol, and from the data analysis. These
conditions include:
- Unanticipated cesarean delivery.
- Performance of episiotomy (third and fourth degree extensions will be excluded).
- Vaginal or cervical laceration, or perineal laceration of more than second degree in
depth.
- Severe postpartum hemorrhage requiring intervention immediately after delivery.
- Uterine rupture
- Placental abruption.
- Patient withdrawal of consent.
Recruitment and Consent Procedures
Patients who meet the inclusion criteria for the study will be identified during their
prenatal clinical visits, in early latent-labor, or prior to induction of labor or active
labor. Informed consent will be obtained by one of the investigators. Consent will be
obtained prior to active labor. The informed consenting process will not be initiated among
patients in active labor. Patients will be recruited and consented with the consent document
approved by the IRB. Patient recruitment will commence after IRB approval is obtained.
Once the subject has consented to participate in the study, it will be determined by the
investigator whether the patient will receive oxytocin alone or oxytocin and misoprostol.
Both drugs are on formulary and will be available on the Labor and Delivery Unit for
immediate use.
Randomization A computer-generated table of random numbers will be used to assign the
recruited subject to a group. A locked file will be maintained in the Labor and Delivery
area. The file will contain a series of sequentially-numbered sealed envelopes. Each envelope
will contain a card with a randomly generated number. These numbers will have been taken in
order from the computer-generated list. The investigator will choose the next envelope in
sequence. If it contains an odd number, the patient will be assigned to the intervention
group and will receive oxytocin and misoprostol. If the envelope contains an even number, the
patient will be assigned to "oxytocin only" group.
Characteristics of Medication Nature of misoprostol Misoprostol is a synthetic prostaglandin
E1 analog. It is marketed primarily as a drug to prevent the development of gastric ulcers
associated with use of nonsteroidal anti-inflammatory drugs, and is part of the Queens
Hospital Center formulary. Originally marketed as Cytotec®, misoprostol is available in a
generic form as tablets containing contain either 100 µg or 200 µg. Misoprostol protects the
gastric mucosa through several mechanisms. It also has the property of stimulating myometrial
smooth muscle contraction.[12] That effect has resulted in the drug's common use in
obstetrics for termination of pregnancy, cervical ripening prior to induction of labor and,
in large doses, for prevention and treatment of postpartum hemorrhage from uterine atony.
[13-19]
Misoprostol can be administered by oral, sublingual, vaginal or rectal routes. It is well
absorbed with all these modes of administration, but detailed pharmacokinetic data exist
primarily concerning its oral administration. It is rapidly absorbed, and undergoes prompt
de-esterification to its free acid, which is responsible for its clinical activity. Peak
plasma levels after oral administration occur after 10-15 min. The half-life is 20-40
minutes. The alpha side chain undergoes beta oxidation and the beta side chain undergoes
omega oxidation followed by reduction of the ketone to give prostaglandin F analogs.
Excretion is primarily in the urine.
Very little misoprostol appears in breast milk. [20,21] After a single 600 µg oral dose of
misoprostol to nursing mothers, misoprostol acid was excreted in breast milk. One hour after
dosing, the milk concentration was about 67% of the maternal serum level; by five hours, the
misoprostol concentrations in breast milk declined to < 1 pg/mL. While no specific data exist
for misoprostol concentrations in colostrum, given the very small ingested volume over the
first few hours of life, neonatal exposure to the drug in the investigator's study can be
expected to be minimal. There are no published reports of adverse effects of misoprostol in
breast-feeding infants of mothers taking misoprostol
Misoprostol is classified by the FDA as a Pregnancy Category X drug. This label is related to
its possible association with congenital anomalies when used in the first trimester, as well
as its abortifacient properties. In the investigator's study, patients will no longer be
pregnant when the participant receives the drug.
The use of misoprostol to enhance uterine activity postpartum is an off-label method, but one
that has gained wide acceptance, and for which there is considerable experience.[8-10, 12-19]
The drug can cause nausea, headache, dyspepsia, vomiting, and constipation or diarrhea with
multiple doses. These side effects are usually mild to moderate and generally subside within
a week. Serious side effects after a single dose are quite rare. In one study of 327 women
who received 600 µg rectally (the dose the investigators propose to use), the most common
side effects were transient shivering (26%) and pyrexia (15%). Both were mild and
short-lived. [16]
Benefits and Risks to Study Subjects There will be no certain medical benefit to the subjects
who participate in the study. It is possible that the participant will benefit from reduced
postpartum blood loss.
Risks to the subjects are those associated with administration or misoprostol. These include
the following adverse events that have been reported in subjects receiving misoprostol for
ulcer prophylaxis: diarrhea, abdominal pain, nausea, flatulence, headache, dyspepsia,
vomiting, and constipation. All occurred in fewer than 5% of patients. Other reported effects
that occurred in clinical trials of misoprostol, but for which no cause-effect relation has
been established included fatigue, fever, chills, rash, alopecia, pallor, breast pain,
abnormal taste, abnormal vision, conjunctivitis, deafness, tinnitus, earache, chest pain,
edema, diaphoresis, hypotension, hypertension, arrhythmia, phlebitis, increased cardiac
enzymes, syncope, myocardial infarction, thromboembolism, abnormal hepatobiliary function,
gingivitis, reflux, dysphagia, gout, polyuria, dysuria, hematuria, urinary tract infection,
anxiety, depression, and thrombocytopenia. As with any drug, anaphylaxis is possible.
The investigators emphasize that in a number of published studies using a single postpartum
dose of misoprostol of 600-1000 µg and including in aggregate in excess of 1000 patients, no
serious side effect has been reported.
Side effects after a single dose of misoprostol are rare. Misoprostol can cause nausea,
headache, heartburn, vomiting, flatulence, and constipation or diarrhea with multiple doses.
These side effects are usually mild to moderate and generally go away within a week. Mild
shivering and slight fever are the most likely side effect of this medication. If side
effects occur, they will probably disappear within an hour.
Oxytocin commonly causes vomiting and nausea. Oxytocin has the potential to cause muscle
contractions. In rare cases, Oxytocin can cause heart palpitations (rapid heartbeat) and
allergic reaction of a rash or swelling.
It is unknown whether Misoprostol and/or Oytocin are excreted in human milk. There is an
unconfirmed relation with Misoprostol and/or Oytocin causing digestive problems, such as
diarrhea, and abdominal cramps in breast-fed newborns. Pariticipants will be advised to
discard breast mild for the first 24 hours to possibly avoid occurrence.
Study Procedure Informed consent will be obtained by one of the investigators or informed
consent delegates. The subject will then be assigned randomly to the control (oxytocin alone)
or the study (oxytocin + misoprostol) group, as described above. The subject and her medical
caretakers will be informed of which group she is in. If the labor eventuates in a vaginal
delivery, all subjects will receive the standard dose of intravenous oxytocin, begun within
one minute of delivery. Subjects in the study group who have not incurred any of the post-hoc
exclusion criteria (episiotomy, major laceration, etc) will receive a dose of 600 µg of
misoprostol in addition to their oxytocin. This will be administered in the form of six 100
µg tablets inserted approximately 2 cm into the anorectal canal by the obstetrician or
midwife who has performed the delivery. The common method for administering Misoprostol for
postpartum hemorrhaging is rectally for local absorption. Since this study is directed toward
prevention instead of treatment, the dosage of 600mg is a lower dosage from the 1000mg
administered, as standard practices, for treating postpartum hemorrhaging of more than 500cc
estimated blood loss. The patient's vital signs will be recorded after delivery according to
standard protocols of the obstetric service. The Data Collection forms will be filled out
after the delivery by one of the investigators. The measurement of postpartum hemoglobin and
hematocrit (H & H) is automatically ordered at 06:00am for all patients who have delivered
the day prior, constituting this measurement at "Postpartum Day 1", which is at a minimum of
6 hours after delivery and is enough time for H & H levels to stabilize.
Within 36 hours of delivery, additional information will be collected from the patient's
record, including the postpartum hemogram and information about any symptoms or signs related
to the misoprostol.
Confidentiality
After a subject has given informed consent, she will be assigned a Study Number. This number
will be used on the study data collection form as the sole patient identifier, i.e., the form
will not contain the subject's name or hospital number. A single hard copy list of the
subjects' Study Numbers and their medical record numbers will be kept in a locked cabinet in
the Principal Investigator's sponsor's office (Dr. Fuks). This list will be destroyed once
the study has been accepted for publication. Only Dr. Fuks will have access to this list.
Costs The cost of each 600 µg dose of misproostol will be $4.80. There will be no charge to
the patient. The drug will be paid for through the research fund of the Department of
Obstetrics and Gynecology at Queens Hospital Center.
Data Collection
Data collection will include the following elements:
Before Delivery
- Age
- Ethnicity/Race
- Gestational age (in weeks)
- Number of previous deliveries
- Number of Fetus
- Body-Mass Index (BMI)
- Amniotic Fluid Index (AFI)
- Cephalic presentation
- Fetal Heart Rate (FHR)
- Reported fetal Anomaly
- Preeclampsia
- Trial of Labor after Cesarean (TOLAC) After Delivery
- Caesarean section (during delivery)
- Epidural
- Oxytocin in labor (if yes, number of hours before delivery
- Other medication used in labor
- Episiotomy
- Duration of stage 1, 2, and 3
- Degree and place of laceration
- Estimated Blood Loss (EBL)
- Transfusion
- Placental Abruption
- Birth weight Results - includes Follow-up Data
- Hemoglobin and Hematocrit (H& H) on admission and on post- partum day #1
- Reported Side effect by patient
- Post partum temperature
- Reports of shivering
- Diagnosis of chorioamnionitis
Post- partum day #1- data collection Postpartum Day 1 is delineated as the first 12:01am
clock time from the time of delivery. Post-partum measurements, such as postpartum hemoglobin
and hematocrit (H & H), are taken automatically at 06:00am for all deliveries that occurred
before midnight (at least 6 hours prior).
estimates indicate that a loss of approximately 500 mL is average, with a range of about
250-700 mL.[1,2] Some of this bleeding arises from birth canal lacerations or surgical
incisions (i.e., episiotomy), but most derives from the vessels exposed in the uterine wall
at the placental site once the placenta has separated.
Under normal circumstances, shortly after placental separation intense myometrial
contractions occur. These raise the pressure within the myometrial wall above that of the
blood pressure in the vessels that traverse it, vessels that opened into the intervillous
space. Flow in these vessels is thus mechanically attenuated by myometrial contraction,
allowing for the formation of intravascular thrombi.
This mechanism for controlling postpartum uterine blood loss works well most of the time. If,
however, the uterus remains hypotonic or atonic after delivery, excessive blood loss can
occur. In the worst cases, severe uterine hemorrhage ensues. Postpartum hemorrhage is, in
fact, the leading cause of maternal mortality in the world, accounting for at least 100,000
deaths annually.[3] Even in the absence of frank hemorrhage, postpartum blood loss can result
in maternal anemia. Recuperation of iron stores to recover from this blood loss takes time,
and may not occur, especially in low socioeconomic areas where dietary iron consumption is
often deficient, and pregnancies tend to occur in close succession.
Postpartum anemia is a significant contributor to short- and long-term morbidity.[5-7] It
increases the risk of infection and poor wound healing. Also, the associated fatigue may
interfere with the mother's ability to administer child care and to bond appropriately with
her infant. Anemic mothers tend to have more difficulty with nursing, and may produce
iron-deficient milk. There is thus a strong rationale to minimize postpartum blood loss.
In most US hospitals, parturients receive a high dose of intravenous or intramuscular
oxytocin immediately after delivery. This approach has been shown in several studies to
reduce the risk of postpartum hemorrhage, [8-11] and is practiced routinely at Queens
Hospital Center. Investigators will employ an intravenous infusion of oxytocin (Pitocin®) at
a rate of about 50-100 mU/minute. Despite this approach, there is still substantial blood
loss at delivery, based on the investigator's preliminary observations shown below. This
provides the rationale to determine whether use of an adjunctive drug, namely misoprostol 600
µg rectally, administered after delivery, might reduce blood loss further than does oxytocin
alone, thus decreasing the risk of morbidity related to postpartum anemia.
Preliminary Data
The investigators examined the hemograms of a randomly chosen consecutive sample of 53
spontaneous vaginal deliveries performed at Queens Hospital Center between September 15 and
October 1, 2010.
Among these patients, the admission hemoglobin concentration was 11.9±1.2 g/dL and that on
the first postparutum day was 10.9±1.3. The mean fall was 1.02 (95% CI 0.74, 1.29), a
statistically significant decrease (P<0.0001). Hematocrit levels fell in parallel, by an
average of 7.8% of the predelivery value. The mean fall in hemoglobin and hematocrit levels
after delivery (1.02 g/dL and 2.81%) is consistent with an average blood loss of about 500
mL. The consistency of these changes and the small associated variance indicate that the
change in hemoglobin and hematocrit levels is a meaningful proxy for the assessment of blood
lost during vaginal delivery.
Study Design The study is a prospective randomized open-label clinical trial to be performed
in a single institution. It will compare the intrapartum and postpartum maternal blood
hemoglobin concentrations and hematocrit measurements in a group of parturients who received
standard prophylactic intravenous oxytocin immediately after delivery with a group that
received oxytocin and adjuvant misoprostol.
Sample size and analysis
A total of 800 subjects will enter this two-treatment parallel design study. With that sample
size, the probability is 90% that the study will detect a treatment difference at a two-sided
0.05 significance level if the difference in hemoglobin concentration between treatments is
0.3 g/dL. This analysis is based on the assumption that the standard deviation of the
postpartum and intrapartum hemoglobin concentrations is not larger than 1.3 g/dL.
Comparison of intrapartum and postpartum hemoglobin and hematocrit levels will be done using
a paired t-test. A probability level of 0.05 will be used as the threshold for significance.
Inclusion and exclusion criteria This study will include adult pregnant women regardless of
age. Pregnant minors under the age of 18 will not be eligible.
A patient will be considered for inclusion in the study if she meets all of the following
criteria:
- She has a term (≥37 completed weeks) live singleton gestation in cephalic presentation
and has been admitted to the Labor and Delivery Unit
- She is in the latent phase of labor or has been admitted for induction of labor or at
prenatal clinic visit
- She has had fewer than four prior vaginal deliveries.
- She reports no allergy to misoprostol.
The following factors or conditions will exclude a patient from consideration as a subject:
- The fetus has a known major fetal malformation or chromosome abnormality
- The gestation is multiple.
- There is a breech or other malpresentation
- The patient reports involvement in another clinical trial currently or previously in
this pregnancy.
- The patient is expected to have a cesarean delivery.
- The patient had a prior cesarean delivery.
- There has been an intrauterine fetal death.
- There is polyhydramnios (amniotic fluid index >22 cm).
- Presence of acute or chronic renal disease
- Presence of preeclampsia
Of subjects who enter the study, the development of certain conditions will exclude them post
hoc from receiving misoprostol under the protocol, and from the data analysis. These
conditions include:
- Unanticipated cesarean delivery.
- Performance of episiotomy (third and fourth degree extensions will be excluded).
- Vaginal or cervical laceration, or perineal laceration of more than second degree in
depth.
- Severe postpartum hemorrhage requiring intervention immediately after delivery.
- Uterine rupture
- Placental abruption.
- Patient withdrawal of consent.
Recruitment and Consent Procedures
Patients who meet the inclusion criteria for the study will be identified during their
prenatal clinical visits, in early latent-labor, or prior to induction of labor or active
labor. Informed consent will be obtained by one of the investigators. Consent will be
obtained prior to active labor. The informed consenting process will not be initiated among
patients in active labor. Patients will be recruited and consented with the consent document
approved by the IRB. Patient recruitment will commence after IRB approval is obtained.
Once the subject has consented to participate in the study, it will be determined by the
investigator whether the patient will receive oxytocin alone or oxytocin and misoprostol.
Both drugs are on formulary and will be available on the Labor and Delivery Unit for
immediate use.
Randomization A computer-generated table of random numbers will be used to assign the
recruited subject to a group. A locked file will be maintained in the Labor and Delivery
area. The file will contain a series of sequentially-numbered sealed envelopes. Each envelope
will contain a card with a randomly generated number. These numbers will have been taken in
order from the computer-generated list. The investigator will choose the next envelope in
sequence. If it contains an odd number, the patient will be assigned to the intervention
group and will receive oxytocin and misoprostol. If the envelope contains an even number, the
patient will be assigned to "oxytocin only" group.
Characteristics of Medication Nature of misoprostol Misoprostol is a synthetic prostaglandin
E1 analog. It is marketed primarily as a drug to prevent the development of gastric ulcers
associated with use of nonsteroidal anti-inflammatory drugs, and is part of the Queens
Hospital Center formulary. Originally marketed as Cytotec®, misoprostol is available in a
generic form as tablets containing contain either 100 µg or 200 µg. Misoprostol protects the
gastric mucosa through several mechanisms. It also has the property of stimulating myometrial
smooth muscle contraction.[12] That effect has resulted in the drug's common use in
obstetrics for termination of pregnancy, cervical ripening prior to induction of labor and,
in large doses, for prevention and treatment of postpartum hemorrhage from uterine atony.
[13-19]
Misoprostol can be administered by oral, sublingual, vaginal or rectal routes. It is well
absorbed with all these modes of administration, but detailed pharmacokinetic data exist
primarily concerning its oral administration. It is rapidly absorbed, and undergoes prompt
de-esterification to its free acid, which is responsible for its clinical activity. Peak
plasma levels after oral administration occur after 10-15 min. The half-life is 20-40
minutes. The alpha side chain undergoes beta oxidation and the beta side chain undergoes
omega oxidation followed by reduction of the ketone to give prostaglandin F analogs.
Excretion is primarily in the urine.
Very little misoprostol appears in breast milk. [20,21] After a single 600 µg oral dose of
misoprostol to nursing mothers, misoprostol acid was excreted in breast milk. One hour after
dosing, the milk concentration was about 67% of the maternal serum level; by five hours, the
misoprostol concentrations in breast milk declined to < 1 pg/mL. While no specific data exist
for misoprostol concentrations in colostrum, given the very small ingested volume over the
first few hours of life, neonatal exposure to the drug in the investigator's study can be
expected to be minimal. There are no published reports of adverse effects of misoprostol in
breast-feeding infants of mothers taking misoprostol
Misoprostol is classified by the FDA as a Pregnancy Category X drug. This label is related to
its possible association with congenital anomalies when used in the first trimester, as well
as its abortifacient properties. In the investigator's study, patients will no longer be
pregnant when the participant receives the drug.
The use of misoprostol to enhance uterine activity postpartum is an off-label method, but one
that has gained wide acceptance, and for which there is considerable experience.[8-10, 12-19]
The drug can cause nausea, headache, dyspepsia, vomiting, and constipation or diarrhea with
multiple doses. These side effects are usually mild to moderate and generally subside within
a week. Serious side effects after a single dose are quite rare. In one study of 327 women
who received 600 µg rectally (the dose the investigators propose to use), the most common
side effects were transient shivering (26%) and pyrexia (15%). Both were mild and
short-lived. [16]
Benefits and Risks to Study Subjects There will be no certain medical benefit to the subjects
who participate in the study. It is possible that the participant will benefit from reduced
postpartum blood loss.
Risks to the subjects are those associated with administration or misoprostol. These include
the following adverse events that have been reported in subjects receiving misoprostol for
ulcer prophylaxis: diarrhea, abdominal pain, nausea, flatulence, headache, dyspepsia,
vomiting, and constipation. All occurred in fewer than 5% of patients. Other reported effects
that occurred in clinical trials of misoprostol, but for which no cause-effect relation has
been established included fatigue, fever, chills, rash, alopecia, pallor, breast pain,
abnormal taste, abnormal vision, conjunctivitis, deafness, tinnitus, earache, chest pain,
edema, diaphoresis, hypotension, hypertension, arrhythmia, phlebitis, increased cardiac
enzymes, syncope, myocardial infarction, thromboembolism, abnormal hepatobiliary function,
gingivitis, reflux, dysphagia, gout, polyuria, dysuria, hematuria, urinary tract infection,
anxiety, depression, and thrombocytopenia. As with any drug, anaphylaxis is possible.
The investigators emphasize that in a number of published studies using a single postpartum
dose of misoprostol of 600-1000 µg and including in aggregate in excess of 1000 patients, no
serious side effect has been reported.
Side effects after a single dose of misoprostol are rare. Misoprostol can cause nausea,
headache, heartburn, vomiting, flatulence, and constipation or diarrhea with multiple doses.
These side effects are usually mild to moderate and generally go away within a week. Mild
shivering and slight fever are the most likely side effect of this medication. If side
effects occur, they will probably disappear within an hour.
Oxytocin commonly causes vomiting and nausea. Oxytocin has the potential to cause muscle
contractions. In rare cases, Oxytocin can cause heart palpitations (rapid heartbeat) and
allergic reaction of a rash or swelling.
It is unknown whether Misoprostol and/or Oytocin are excreted in human milk. There is an
unconfirmed relation with Misoprostol and/or Oytocin causing digestive problems, such as
diarrhea, and abdominal cramps in breast-fed newborns. Pariticipants will be advised to
discard breast mild for the first 24 hours to possibly avoid occurrence.
Study Procedure Informed consent will be obtained by one of the investigators or informed
consent delegates. The subject will then be assigned randomly to the control (oxytocin alone)
or the study (oxytocin + misoprostol) group, as described above. The subject and her medical
caretakers will be informed of which group she is in. If the labor eventuates in a vaginal
delivery, all subjects will receive the standard dose of intravenous oxytocin, begun within
one minute of delivery. Subjects in the study group who have not incurred any of the post-hoc
exclusion criteria (episiotomy, major laceration, etc) will receive a dose of 600 µg of
misoprostol in addition to their oxytocin. This will be administered in the form of six 100
µg tablets inserted approximately 2 cm into the anorectal canal by the obstetrician or
midwife who has performed the delivery. The common method for administering Misoprostol for
postpartum hemorrhaging is rectally for local absorption. Since this study is directed toward
prevention instead of treatment, the dosage of 600mg is a lower dosage from the 1000mg
administered, as standard practices, for treating postpartum hemorrhaging of more than 500cc
estimated blood loss. The patient's vital signs will be recorded after delivery according to
standard protocols of the obstetric service. The Data Collection forms will be filled out
after the delivery by one of the investigators. The measurement of postpartum hemoglobin and
hematocrit (H & H) is automatically ordered at 06:00am for all patients who have delivered
the day prior, constituting this measurement at "Postpartum Day 1", which is at a minimum of
6 hours after delivery and is enough time for H & H levels to stabilize.
Within 36 hours of delivery, additional information will be collected from the patient's
record, including the postpartum hemogram and information about any symptoms or signs related
to the misoprostol.
Confidentiality
After a subject has given informed consent, she will be assigned a Study Number. This number
will be used on the study data collection form as the sole patient identifier, i.e., the form
will not contain the subject's name or hospital number. A single hard copy list of the
subjects' Study Numbers and their medical record numbers will be kept in a locked cabinet in
the Principal Investigator's sponsor's office (Dr. Fuks). This list will be destroyed once
the study has been accepted for publication. Only Dr. Fuks will have access to this list.
Costs The cost of each 600 µg dose of misproostol will be $4.80. There will be no charge to
the patient. The drug will be paid for through the research fund of the Department of
Obstetrics and Gynecology at Queens Hospital Center.
Data Collection
Data collection will include the following elements:
Before Delivery
- Age
- Ethnicity/Race
- Gestational age (in weeks)
- Number of previous deliveries
- Number of Fetus
- Body-Mass Index (BMI)
- Amniotic Fluid Index (AFI)
- Cephalic presentation
- Fetal Heart Rate (FHR)
- Reported fetal Anomaly
- Preeclampsia
- Trial of Labor after Cesarean (TOLAC) After Delivery
- Caesarean section (during delivery)
- Epidural
- Oxytocin in labor (if yes, number of hours before delivery
- Other medication used in labor
- Episiotomy
- Duration of stage 1, 2, and 3
- Degree and place of laceration
- Estimated Blood Loss (EBL)
- Transfusion
- Placental Abruption
- Birth weight Results - includes Follow-up Data
- Hemoglobin and Hematocrit (H& H) on admission and on post- partum day #1
- Reported Side effect by patient
- Post partum temperature
- Reports of shivering
- Diagnosis of chorioamnionitis
Post- partum day #1- data collection Postpartum Day 1 is delineated as the first 12:01am
clock time from the time of delivery. Post-partum measurements, such as postpartum hemoglobin
and hematocrit (H & H), are taken automatically at 06:00am for all deliveries that occurred
before midnight (at least 6 hours prior).
A patient will be considered for inclusion in the study if she meets all of the following
criteria:
- She has a term (≥37 completed weeks) live singleton gestation in cephalic presentation
and has been admitted to the Labor and Delivery Unit
- She is in the latent phase of labor or has been admitted for induction of labor or at
prenatal clinic visit
- She has had fewer than four prior vaginal deliveries.
- She reports no allergy to misoprostol.
The following factors or conditions will exclude a patient from consideration as a subject:
- The fetus has a known major fetal malformation or chromosome abnormality
- The gestation is multiple.
- There is a breech or other malpresentation
- The patient reports involvement in another clinical trial currently or previously in
this pregnancy.
- The patient is expected to have a cesarean delivery.
- The patient had a prior cesarean delivery.
- There has been an intrauterine fetal death.
- There is polyhydramnios (amniotic fluid index >22 cm).
- Presence of acute or chronic renal disease
- Presence of preeclampsia
Of subjects who enter the study, the development of certain conditions will exclude them
post hoc from receiving misoprostol under the protocol, and from the data analysis. These
conditions include:
- Unanticipated cesarean delivery.
- Performance of episiotomy (third and fourth degree extensions will be excluded).
- Vaginal or cervical laceration, or perineal laceration of more than second degree in
depth.
- Severe postpartum hemorrhage requiring intervention immediately after delivery.
- Uterine rupture
- Placental abruption.
- Patient withdrawal of consent.
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