Effectiveness and safety of misoprostol distributed to antenatal women to prevent postpartum haemorrhage after child-births: A stepped-wedge cluster-randomized trial

BMC Pregnancy and Childbirth, Volume 15, No. 1, Year 2015

Interpretação

Background: Oral misoprostol, administered by trained health-workers is effective and safe for preventing postpartum haemorrhage (PPH). There is interest in expanding administration of misoprostol by non-health workers, including task-shifting to pregnant women themselves. However, the use of misoprostol for preventing PPH in home-births remains controversial, due to the limited evidence to support self-administration or leaving it in the hands of non-health workers. This study aimed to determine if antenatally distributing misoprostol to pregnant women to self-administer at home birth reduces PPH. Methods: Between February 2013 and March 2014, we conducted a stepped-wedge cluster-randomized trial in six health facilities in Central Uganda. Women at 28+ weeks of gestation attending antenatal care were eligible. Women in the control-arm received the standard-of-care; while the intervention-arm were offered 600mcg of misoprostol to swallow immediately after birth of baby, when oxytocin was not available. The primary outcome (PPH) was a drop in postpartum maternal haemoglobin (Hb) by ≥2g/dl, lower than the prenatal Hb. Analysis was by intention-to-treat at the cluster level and we used a paired t-tests to assess whether the mean difference between the control and intervention groups was statistically significant. Results: 97% (2466/2545) of eligible women consented to participate; 1430 and 1036 in the control and intervention arms respectively. Two thousand fifty-seven of the participants were successfully followed up and 271(13.2%) delivered outside a health facility. There was no significant difference between the study group in number of women who received a uterotonic at birth (control 80.4% vs intervention 91.4%, mean difference=-11.0%, 95% confidence interval [CI] -25.7% to 3.6%, p=0.11). No woman took misoprostol before their baby’s birth. Shivering and fever were 14.9% in the control arm compared to 22.2% in the intervention arm (mean difference=-7.2%, 95%CI -11.1% to -3.7%), p=0.005). There was a slight, but non-significant, reduction in the percentage of women with Hb drop ≥2g/dl from 18.5% in the control arm to 11.4% in the intervention arm (mean difference=7.1%, 95%CI -3.1% to 17.3%, p=0.14). Similarly, there was no significant difference between the groups in the primary outcome in the women who delivered at home (control 9.6% vs intervention 14.5%, mean difference -4.9; 95% CI -12.7 to 2.9), p=0.17). Conclusion: This study was unable to detect a significant reduction in PPH following the antenatal distribution of misoprostol. The study was registered with Pan-African Clinical Trials Network ( PACTR201303000459148 , on 19/11/2012). Ethical approval was obtained from the School of Medicine Research and Ethics Committee at Makerere University, Kampala, Uganda, and the Uganda National Council for Science and Technology. Permission to carry out the study was obtained from the District Health Office (DHO) and respective in-charges of the health facilities. After information and counselling, eligible women provided written informed consent and received an information sheet in either English or Luganda. The study was registered with the Pan African Clinical Trials Network (PACTR201303000459148) on 19/11/2012. We employed a stepped-wedge cluster-randomized trial design [22] because current evidence on misoprostol use and postpartum haemorrhage would render a placebo-controlled trial unethical [19, 22–25] and all facilities ultimately get the intervention. A cluster was defined as a health facility catchment area. All health facilities started as control-arm facilities. Then in a prior-determined random order, two facilities “crossed over” to become intervention facilities during each of the subsequent three steps for a total of four steps (Fig. 1). Stepped-wedge schema for the trial. Six clusters were enrolled at baseline. The white (non-shaded) cells marked “C” represent the control period. The gray (shaded) cells marked “I” represent the intervention period The random sequence for starting the intervention was determined before the start of the study by using computer generated number sequence. The principal investigator implemented the randomization. Each step lasted for two months, and women were followed up on 3rd to 5th day post delivered. Because of the nature of the intervention, it was not possible to blind the intervention to the care-givers, research team or study participants. The study participants were recruited from six health facilities in Mpigi district, Uganda, between February 2013 and March 2014. The majority of people in the district are of low socioeconomic status, with peasant farming and fishing as their main economic activities. The district health infrastructure consisted of 31 health units (25 government and 6 non-government). These included one private hospital, one Health Centre IV, 13 Health Centre IIIs, and 16 Health Centre IIs. The district recorded a skilled birth attendant rate of 30 % (2010–11 District Annual Report), although the national average was 58 % [21]. We enrolled study participants at the antenatal clinic of the Health Centre IV and the five Health Centre IIIs. Two health facilities held their antenatal clinics from Monday to Friday, while the other four had two dedicated antenatal-care service days per week. Maternity services at the Health Centre IIIs were staffed by midwives, while the Health Centre IV had three medical officers in addition to the 7 midwives, and provided comprehensive emergency obstetric care. The staff in the antenatal clinic and delivery wards were involved in recruiting and following up the women, which allowed the intervention to be delivered as part of ongoing maternity care. Clinics: All the 31 health facilities were screened for eligibility. The eligibility criteria were a) that a minimum of 50 pregnant women attended antenatal clinic (for the first time) in the month prior to the start of the study, and b) that the person in-charge of health facility agreed for the facility to participate. Of the nine facilities that registered a minimum of 50 antenatal first-time attendees per month, we excluded three; the hospital because health-care services are paid for (private hospital); one health facility because its in-charge declined to participate; and another because it was difficult to access the women after home birth during the wet season due to seasonal rivers and swamps. Women: Within the antenatal clinics of participating health facilities, we included all pregnant women who were 28 weeks or more of gestation, and who had no plans to leave the district during pregnancy delivery or in the immediate postpartum period. We excluded women who had a planned elective caesarean-section delivery or previous caesarean section scars. Study staff briefed pregnant women attending the antenatal clinic about the study objectives and design of the study in a group. The key messages to the pregnant women included: 1. The benefits of delivering at the health facility, 2. Excessive bleeding after child-birth was dangerous to a woman’s life, 3. The availability of an effective drug (oxytocin) to stop excessive bleeding that can be given by trained health worker at the time of birth in the health facility. 4. For those willing to participate, the need to alert the research assistant by telephone when and where the delivery occurred. We repeated the sessions about the study in every antenatal clinic throughout the study period (in both control and intervention phases). After the discussion, we invited those eligible to participate. Each participant gave a written informed consent. At the time of the trial, the standard-of-care was that a women who delivered at a health facility should receive oxytocin to prevent PPH, while women who delivered at home received no uterotonic. Women in the intervention period were given 600 micrograms (mcg) of oral misoprostol at enrolment to the study to self-administer after childbirth if delivery happened outside a health facility, or when there was no oxytocin at the health facility. The three tablets of misoprostol (200 mcg each for a total of 600mcg) in aluminum foil were packaged in a plastic envelope. Women were given the following instructions; “1. Not to take the misoprostol tablets when the baby is still inside the womb, 2. To swallow all the three tablets immediately after the birth of the baby, if delivery occurred at home, or if no oxytocin was given by the health provider. If she had twins, she was to swallow the tablets after the birth of second twin. 3. To keep the packaging of tablets (foil) after swallowing them and to give it to research assistant when she visits her. 4. To carry along the study tablets (misoprostol) when going to deliver at a health facility. Hand the misoprostol tablets to the attending midwife or research assistant if delivery occurred at health facility.” The research assistants and health facility staff in the antenatal clinics and delivery wards from the six study facilities were trained on the protocol for 5 h. This comprised of study material and key messages to women attending antenatal clinic, and was delivered by the principal investigator. Weekly supervisory visits by the principal investigator followed the initial training and further training was given as requested or as assessed by the principal investigator. The study participants were interviewed face-to-face by a trained research assistant. We used a pre-tested questionnaire to collect socio-demographic characteristics including maternal age, education, marital status, maternal occupation and religious affiliation. We also inquired about parity, gestation at first antenatal visit, the use of prophylactic anti-malarials, transport costs to the health facility for antenatal care, and delivery plans. We established gestational age from the woman’s last normal menstrual period (LNMP) or ultrasound scan estimation. In a few cases where we did not have LNMP or an ultrasound scan, we used fundal height to approximate the gestational age [26]. Trained research assistants measured haemoglobin (Hb) levels at enrolment (during their third trimester antenatal care visit) and three to five days after delivery using a portable HemoCueR Hb 301 system. as described in another part of the study that looked at haemoglobin status of pregnant women [27]. All pregnant women enrolled in the study continued receiving standard antenatal care at the local health facility. A sticker identifying them as enrolled study participants was placed on their hand-held antenatal cards to make it easier to identify them at repeat antenatal visits or when they reported in labour. The sticker had three telephone numbers that the women could call to contact the study team once they had delivered or if they had any problems or questions about study. At enrolment, women were advised to deliver in a health facility as per national guidelines. They were also advised to seek care in case they had excessive bleeding after child birth, the placenta had not delivered within one hour, or the baby did not cry immediately after birth or developed a fever. The study kept a log of participants’ names, contact telephone numbers and the name of the village health worker where they lived. The study team contacted any woman who had passed her estimated delivery date to identify if she had given birth and from where. Midway through the study, we observed that the names of participants in the log book were often not what the women were called by the community members in the village, so we subsequently modified our procedures to ask participants for the names (petty names) the community members usually called them. Research assistants visited the woman either at home or at the health facility after birth to measure the haemoglobin and complete postnatal questionnaire. Participants were defined as lost-to-follow-up when we were unable to physically contact them eight weeks after the expected date of delivery. The primary outcome was PPH, defined as a drop in maternal haemoglobin by 2g/dl or more, lower than the prenatal Hb [10]. Secondary outcomes were: postpartum anaemia defined as Hb < 11 g/dl when assessed within 7 days and Hb < 12 g/dl if assessed after the 7th day after childbirth [28], place of child-birth, use of any uterotonics for prevention of PPH, referral to a health facility after delivery, blood transfusion and maternal death. We asked the women about side effects related to misoprostol use, such as fever (self-report of body feeling hot), chills, shivering and how they coped with them. Safety was defined as swallowing of the medicine after delivery of the baby or babies. Specific to the intervention group, we also assessed the timing of swallowing misoprostol, and its acceptability to women. We asked the women in the intervention group to keep the blister package of the misoprostol (used or unused) and hand it to research assistant at home during the follow up visit or to the nurse at the health facility where the woman delivered. Sample size was calculated taking into account the clustering effect. We assumed a between cluster correlation coefficient km = 0.2, a minimum of 200 pregnant women per health facility in each phase (m), and proportion experiencing PPH of 12.0 % [9]. Assuming 80 % power to detect a difference of 50 % in PPH proportions between the two groups with a type I error of 5 %, using formula for matched cluster trial [29], the study needed six health facilities in each arm, Analysis was conducted on an intention-to-treat principle, based on the period (intervention or control) at which women were enrolled into the study. We compared the characteristics of women enrolled in the control and the intervention periods at individual level and these were summarized as percentages for categorical outcomes, and means (and standard deviations) for continuous outcomes. Cluster-level summaries of some women’s characteristics in the control and intervention periods were computed and presented as means and standard deviations. The primary outcome (postpartum Hb ≥ 2g/dl lower than prenatal Hb) in each arm was expressed as the mean of the six cluster-level proportions of women who had PPH measured in each cluster in intervention and control periods respectively. The effect of the intervention was measured as the difference in the means of primary outcome of the two groups (with 95 % confidence interval [CI]). We used paired t-tests to assess whether the mean difference between the two groups was statistically different from zero. We also applied a paired t-test to assess the difference in the means of the secondary outcomes between the control and intervention groups. Uterotonic use included a summary statistic of uterotonic received at birth and was cross-tabulated with place of birth. The acceptability of misoprostol as a number of home births who ingested misoprostol and were willing to use it next pregnancy or recommend it to relative. Results were summarized as frequency distribution. Because the study did not have a lag phase, some of women recruited during the control period delivered in the intervention period.

AI Digest

Study Justification:

– The study aimed to determine if distributing misoprostol to pregnant women for self-administration at home birth reduces postpartum hemorrhage (PPH).
– There is interest in expanding the use of misoprostol by non-health workers, including pregnant women themselves, but limited evidence exists to support this practice.
– The study aimed to provide evidence on the effectiveness and safety of misoprostol distribution to pregnant women.

Study Highlights:

– The study was conducted in six health facilities in Central Uganda between February 2013 and March 2014.
– A total of 2,466 eligible women participated in the study, with 1,430 in the control arm and 1,036 in the intervention arm.
– The primary outcome, PPH, was defined as a drop in postpartum maternal hemoglobin (Hb) by ≥2g/dl, lower than the prenatal Hb.
– There was no significant difference in the number of women who received a uterotonic at birth between the control and intervention groups.
– Shivering and fever were more common in the intervention arm compared to the control arm.
– There was a slight reduction in the percentage of women with Hb drop ≥2g/dl in the intervention arm, but it was not statistically significant.
– There was no significant difference in the primary outcome for women who delivered at home.

Recommendations for Lay Reader and Policy Maker:

– The study did not find a significant reduction in postpartum hemorrhage following the distribution of misoprostol to pregnant women for self-administration at home birth.
– Further research is needed to determine the effectiveness and safety of this practice.
– Policy makers should consider the limitations of the current evidence and carefully evaluate the potential risks and benefits before implementing widespread distribution of misoprostol to pregnant women.

Key Role Players:

– Trained health workers
– Pregnant women
– Research assistants
– Health facility staff (antenatal clinics and delivery wards)
– Principal investigator

Cost Items for Planning Recommendations:

– Training materials and sessions for health facility staff and research assistants
– Portable HemoCueR Hb 301 system for measuring hemoglobin levels
– Packaging and distribution of misoprostol tablets
– Transportation costs for research assistants to visit participants
– Data collection and analysis
– Monitoring and supervision by the principal investigator

Força da prova

N/A

Resumo

Ethical approval was obtained from the School of Medicine Research and Ethics Committee at Makerere University, Kampala, Uganda, and the Uganda National Council for Science and Technology. Permission to carry out the study was obtained from the District Health Office (DHO) and respective in-charges of the health facilities. After information and counselling, eligible women provided written informed consent and received an information sheet in either English or Luganda. The study was registered with the Pan African Clinical Trials Network (PACTR201303000459148) on 19/11/2012. We employed a stepped-wedge cluster-randomized trial design [22] because current evidence on misoprostol use and postpartum haemorrhage would render a placebo-controlled trial unethical [19, 22–25] and all facilities ultimately get the intervention. A cluster was defined as a health facility catchment area. All health facilities started as control-arm facilities. Then in a prior-determined random order, two facilities “crossed over” to become intervention facilities during each of the subsequent three steps for a total of four steps (Fig. 1). Stepped-wedge schema for the trial. Six clusters were enrolled at baseline. The white (non-shaded) cells marked “C” represent the control period. The gray (shaded) cells marked “I” represent the intervention period The random sequence for starting the intervention was determined before the start of the study by using computer generated number sequence. The principal investigator implemented the randomization. Each step lasted for two months, and women were followed up on 3rd to 5th day post delivered. Because of the nature of the intervention, it was not possible to blind the intervention to the care-givers, research team or study participants. The study participants were recruited from six health facilities in Mpigi district, Uganda, between February 2013 and March 2014. The majority of people in the district are of low socioeconomic status, with peasant farming and fishing as their main economic activities. The district health infrastructure consisted of 31 health units (25 government and 6 non-government). These included one private hospital, one Health Centre IV, 13 Health Centre IIIs, and 16 Health Centre IIs. The district recorded a skilled birth attendant rate of 30 % (2010–11 District Annual Report), although the national average was 58 % [21]. We enrolled study participants at the antenatal clinic of the Health Centre IV and the five Health Centre IIIs. Two health facilities held their antenatal clinics from Monday to Friday, while the other four had two dedicated antenatal-care service days per week. Maternity services at the Health Centre IIIs were staffed by midwives, while the Health Centre IV had three medical officers in addition to the 7 midwives, and provided comprehensive emergency obstetric care. The staff in the antenatal clinic and delivery wards were involved in recruiting and following up the women, which allowed the intervention to be delivered as part of ongoing maternity care. Clinics: All the 31 health facilities were screened for eligibility. The eligibility criteria were a) that a minimum of 50 pregnant women attended antenatal clinic (for the first time) in the month prior to the start of the study, and b) that the person in-charge of health facility agreed for the facility to participate. Of the nine facilities that registered a minimum of 50 antenatal first-time attendees per month, we excluded three; the hospital because health-care services are paid for (private hospital); one health facility because its in-charge declined to participate; and another because it was difficult to access the women after home birth during the wet season due to seasonal rivers and swamps. Women: Within the antenatal clinics of participating health facilities, we included all pregnant women who were 28 weeks or more of gestation, and who had no plans to leave the district during pregnancy delivery or in the immediate postpartum period. We excluded women who had a planned elective caesarean-section delivery or previous caesarean section scars. Study staff briefed pregnant women attending the antenatal clinic about the study objectives and design of the study in a group. The key messages to the pregnant women included: 1. The benefits of delivering at the health facility, 2. Excessive bleeding after child-birth was dangerous to a woman’s life, 3. The availability of an effective drug (oxytocin) to stop excessive bleeding that can be given by trained health worker at the time of birth in the health facility. 4. For those willing to participate, the need to alert the research assistant by telephone when and where the delivery occurred. We repeated the sessions about the study in every antenatal clinic throughout the study period (in both control and intervention phases). After the discussion, we invited those eligible to participate. Each participant gave a written informed consent. At the time of the trial, the standard-of-care was that a women who delivered at a health facility should receive oxytocin to prevent PPH, while women who delivered at home received no uterotonic. Women in the intervention period were given 600 micrograms (mcg) of oral misoprostol at enrolment to the study to self-administer after childbirth if delivery happened outside a health facility, or when there was no oxytocin at the health facility. The three tablets of misoprostol (200 mcg each for a total of 600mcg) in aluminum foil were packaged in a plastic envelope. Women were given the following instructions; “1. Not to take the misoprostol tablets when the baby is still inside the womb, 2. To swallow all the three tablets immediately after the birth of the baby, if delivery occurred at home, or if no oxytocin was given by the health provider. If she had twins, she was to swallow the tablets after the birth of second twin. 3. To keep the packaging of tablets (foil) after swallowing them and to give it to research assistant when she visits her. 4. To carry along the study tablets (misoprostol) when going to deliver at a health facility. Hand the misoprostol tablets to the attending midwife or research assistant if delivery occurred at health facility.” The research assistants and health facility staff in the antenatal clinics and delivery wards from the six study facilities were trained on the protocol for 5 h. This comprised of study material and key messages to women attending antenatal clinic, and was delivered by the principal investigator. Weekly supervisory visits by the principal investigator followed the initial training and further training was given as requested or as assessed by the principal investigator. The study participants were interviewed face-to-face by a trained research assistant. We used a pre-tested questionnaire to collect socio-demographic characteristics including maternal age, education, marital status, maternal occupation and religious affiliation. We also inquired about parity, gestation at first antenatal visit, the use of prophylactic anti-malarials, transport costs to the health facility for antenatal care, and delivery plans. We established gestational age from the woman’s last normal menstrual period (LNMP) or ultrasound scan estimation. In a few cases where we did not have LNMP or an ultrasound scan, we used fundal height to approximate the gestational age [26]. Trained research assistants measured haemoglobin (Hb) levels at enrolment (during their third trimester antenatal care visit) and three to five days after delivery using a portable HemoCueR Hb 301 system. as described in another part of the study that looked at haemoglobin status of pregnant women [27]. All pregnant women enrolled in the study continued receiving standard antenatal care at the local health facility. A sticker identifying them as enrolled study participants was placed on their hand-held antenatal cards to make it easier to identify them at repeat antenatal visits or when they reported in labour. The sticker had three telephone numbers that the women could call to contact the study team once they had delivered or if they had any problems or questions about study. At enrolment, women were advised to deliver in a health facility as per national guidelines. They were also advised to seek care in case they had excessive bleeding after child birth, the placenta had not delivered within one hour, or the baby did not cry immediately after birth or developed a fever. The study kept a log of participants’ names, contact telephone numbers and the name of the village health worker where they lived. The study team contacted any woman who had passed her estimated delivery date to identify if she had given birth and from where. Midway through the study, we observed that the names of participants in the log book were often not what the women were called by the community members in the village, so we subsequently modified our procedures to ask participants for the names (petty names) the community members usually called them. Research assistants visited the woman either at home or at the health facility after birth to measure the haemoglobin and complete postnatal questionnaire. Participants were defined as lost-to-follow-up when we were unable to physically contact them eight weeks after the expected date of delivery. The primary outcome was PPH, defined as a drop in maternal haemoglobin by 2g/dl or more, lower than the prenatal Hb [10]. Secondary outcomes were: postpartum anaemia defined as Hb < 11 g/dl when assessed within 7 days and Hb < 12 g/dl if assessed after the 7th day after childbirth [28], place of child-birth, use of any uterotonics for prevention of PPH, referral to a health facility after delivery, blood transfusion and maternal death. We asked the women about side effects related to misoprostol use, such as fever (self-report of body feeling hot), chills, shivering and how they coped with them. Safety was defined as swallowing of the medicine after delivery of the baby or babies. Specific to the intervention group, we also assessed the timing of swallowing misoprostol, and its acceptability to women. We asked the women in the intervention group to keep the blister package of the misoprostol (used or unused) and hand it to research assistant at home during the follow up visit or to the nurse at the health facility where the woman delivered. Sample size was calculated taking into account the clustering effect. We assumed a between cluster correlation coefficient km = 0.2, a minimum of 200 pregnant women per health facility in each phase (m), and proportion experiencing PPH of 12.0 % [9]. Assuming 80 % power to detect a difference of 50 % in PPH proportions between the two groups with a type I error of 5 %, using formula for matched cluster trial [29], the study needed six health facilities in each arm, Analysis was conducted on an intention-to-treat principle, based on the period (intervention or control) at which women were enrolled into the study. We compared the characteristics of women enrolled in the control and the intervention periods at individual level and these were summarized as percentages for categorical outcomes, and means (and standard deviations) for continuous outcomes. Cluster-level summaries of some women’s characteristics in the control and intervention periods were computed and presented as means and standard deviations. The primary outcome (postpartum Hb ≥ 2g/dl lower than prenatal Hb) in each arm was expressed as the mean of the six cluster-level proportions of women who had PPH measured in each cluster in intervention and control periods respectively. The effect of the intervention was measured as the difference in the means of primary outcome of the two groups (with 95 % confidence interval [CI]). We used paired t-tests to assess whether the mean difference between the two groups was statistically different from zero. We also applied a paired t-test to assess the difference in the means of the secondary outcomes between the control and intervention groups. Uterotonic use included a summary statistic of uterotonic received at birth and was cross-tabulated with place of birth. The acceptability of misoprostol as a number of home births who ingested misoprostol and were willing to use it next pregnancy or recommend it to relative. Results were summarized as frequency distribution. Because the study did not have a lag phase, some of women recruited during the control period delivered in the intervention period.

Materiais

https://efashare.b-cdn.net/materials/6e02a18e0f0bb1b9693fe07c19ac1e9fe6d439757d3c800338ea5311ccc3a7b8/12884_2015_750_MOESM1_ESM.docx

Inovações

Based on the provided information, one potential innovation to improve access to maternal health is the antenatal distribution of misoprostol to pregnant women for self-administration at home births. This innovation aims to prevent postpartum hemorrhage (PPH), a major cause of maternal mortality. The study conducted a stepped-wedge cluster-randomized trial in Central Uganda to determine the effectiveness and safety of this approach. The results of the study showed that there was no significant reduction in PPH following the antenatal distribution of misoprostol. However, further research and evaluation may be needed to explore the potential benefits and challenges of this innovation in different settings.

AI Innovations Description

The recommendation based on the study is to further explore the use of misoprostol distributed to antenatal women for self-administration at home births to prevent postpartum hemorrhage (PPH). The study found that there was no significant reduction in PPH following the antenatal distribution of misoprostol. However, there was a slight, non-significant reduction in the percentage of women with a drop in postpartum maternal hemoglobin (Hb) by ≥2g/dl, lower than the prenatal Hb.

To develop this recommendation into an innovation to improve access to maternal health, further research and evaluation should be conducted. This could include conducting larger-scale trials to gather more robust evidence on the effectiveness and safety of self-administered misoprostol for preventing PPH in home births. Additionally, efforts should be made to address any concerns or controversies surrounding the use of misoprostol by non-health workers, such as pregnant women themselves. This could involve developing clear guidelines and protocols for the distribution and use of misoprostol, as well as providing training and support for pregnant women who choose to self-administer the medication.

Furthermore, it may be beneficial to explore the integration of misoprostol distribution into existing antenatal care services, ensuring that pregnant women are adequately informed about the benefits and potential risks of using misoprostol for preventing PPH. This could involve incorporating education and counseling sessions into antenatal care visits, as well as providing ongoing support and monitoring for women who choose to use misoprostol.

Overall, the recommendation is to continue exploring the use of misoprostol distributed to antenatal women for self-administration at home births as a potential strategy to improve access to maternal health and prevent postpartum hemorrhage. This should be done through further research, evaluation, and the development of clear guidelines and protocols.

AI Innovations Methodology

Based on the provided information, one potential recommendation to improve access to maternal health is to explore alternative methods of distributing misoprostol to pregnant women for preventing postpartum hemorrhage (PPH) after childbirth. This could involve task-shifting to pregnant women themselves, allowing them to self-administer misoprostol at home births when oxytocin is not available.

To simulate the impact of this recommendation on improving access to maternal health, a methodology could be developed as follows:

1. Study Design: Conduct a stepped-wedge cluster-randomized trial, similar to the one described in the provided description. This design allows for the gradual implementation of the intervention in different clusters (health facilities) over time, while still maintaining a control group for comparison.

2. Selection of Clusters: Identify a suitable number of health facilities in the target area to participate in the trial. Consider factors such as accessibility, availability of trained health workers, and willingness to participate.

3. Randomization: Randomly assign the selected health facilities to either the control or intervention group. This can be done using computer-generated number sequences to ensure unbiased allocation.

4. Intervention Implementation: In the intervention group, pregnant women attending antenatal care would be offered 600mcg of misoprostol to self-administer immediately after the birth of their baby, when oxytocin is not available. The control group would receive standard-of-care without misoprostol distribution.

5. Data Collection: Collect data on various outcomes, including the primary outcome of PPH (defined as a drop in postpartum maternal hemoglobin by ≥2g/dl lower than the prenatal hemoglobin). Secondary outcomes may include postpartum anemia, place of childbirth, use of uterotonics, referral to a health facility, blood transfusion, and maternal death.

6. Follow-up and Monitoring: Follow up with the study participants to assess the impact of the intervention on the outcomes of interest. This can be done through home visits or scheduled clinic visits, depending on the context and resources available.

7. Data Analysis: Analyze the collected data using appropriate statistical methods, such as paired t-tests, to compare the outcomes between the control and intervention groups. Calculate mean differences, confidence intervals, and p-values to determine the statistical significance of the findings.

8. Ethical Considerations: Obtain ethical approval from relevant research ethics committees and ensure informed consent from all study participants. Adhere to ethical guidelines and protect the privacy and confidentiality of the participants.

9. Dissemination of Results: Share the findings of the study through scientific publications, conferences, and other relevant platforms to contribute to the body of knowledge on improving access to maternal health.

By following this methodology, the impact of distributing misoprostol to pregnant women for preventing PPH can be simulated and evaluated, providing valuable insights into its effectiveness and safety in improving access to maternal health.

Autor

Dima Health

Statistics:

Citations: 14

Identifiers:

DOI: 10.1186/s12884-015-0750-6

Research Areas:

Community Interventions, Disability, Health System and Policy, Maternal Access, Maternal and Child Health, Quality of Care, Sexual and Reproductive Health, Social Determinants, Technology and Innovations, Workforce

Study Countries:

Uganda

Study Design:

Cohort Study, randomised-control-trial

Participants Gender:

Female

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