Views among Malawian women about joining HIV prevention clinical trials when pregnant

AIDS Research and Therapy, Volume 17, No. 1, Year 2020

Interpretação

Background: The pressing need to expand the biomedical HIV prevention evidence base during pregnancy is now increasingly recognized. Women’s views regarding participation in such trials and initiating PrEP while pregnant are critical to inform evolving policy and best practices aimed at responsibly expanding evidence-based access for this population. Methods: We conducted 35 semi-structured interviews with reproductive-aged women in Malawi in the local language, Chichewa. Participants were HIV-negative and purposively sampled to capture a range of experience with research during pregnancy. Women’s perspectives on enrolling in three hypothetical HIV prevention trial vignettes while pregnant were explored, testing: (1) oral PrEP (Truvada) (2) a vaginal ring (dapivirine), and (3) a randomized trial comparing the two. The vignettes were read aloud to participants and a simple visual was provided. Interviews were audio-recorded, transcribed, translated, and coded using NVivo 11. Thematic analysis informed the analytic approach. Results: A majority of women accepted participation in all trials. Women’s views on research participation varied largely based on their assessment of whether participation or nonparticipation would best protect their own health and that of their offspring. Women interested in participating described power dynamics with their partner as fueling their HIV exposure concerns and highlighted health benefits of participation – principally, HIV protection and access to testing/treatment and ancillary care, and perceived potential risks of the vignettes as low. Women who were uninterested in participating highlighted potential maternal and fetal health risks of the trial, challenges of justifying prevention use to their partner, and raised some modality-specific concerns. Women also described ways their social networks, sense of altruism and adherence requirements would influence participation decisions. Conclusions: The majority of participants conveyed strong interest in participating in biomedical HIV prevention research during pregnancy, largely motivated by a desire to protect themselves and their offspring. Our results are consistent with other studies that found high acceptance of HIV prevention products during pregnancy, and support the current direction of HIV research policies and practices that are increasingly aimed at protecting the health of pregnant women and their offspring through responsible research, rather than defaulting to their exclusion. The data for this analysis were collected in partnership with UNC Project Malawi and as part of a larger project, Pregnancy and HIV/AIDS: Seeking Equitable Study (PHASES). We conducted qualitative, in-depth interviews using a semi-structured guide to assess the views of women who might be eligible to participate in HIV research during pregnancy about (1) their experiences with research; (2) selected rules governing the intersection of research and reproduction; and (3) their responses to theoretical vignettes describing research during pregnancy. The latter are reported here. Participants included in this analysis were all HIV-negative, and purposively sampled to capture a range of experience with research during pregnancy. UNC Project Malawi in Lilongwe is a study site for U.S. National Institute of Allergy and Infectious Diseases (NIAID) HIV/AIDS Clinical Trials Network studies, many of which involve women of reproductive age. Just over half of the sample (see Table 2) were either: (1) women who had previously participated in a biomedical HIV prevention trial during pregnancy, or (2) women who were denied enrollment in a biomedical HIV prevention trial due to pregnancy; women meeting either criterion are described here as “research experienced”. Research experienced participants were identified by Malawi based research outreach staff through existing trial participation records at UNC Project Malawi. For this purposively selected research experienced subsample, current pregnancy status was not an eligibility requirement. Outreach staff contacted the women by phone, provided a brief description of the study, and invited them to participate. Those who indicated interest were scheduled for an interview appointment in a private office used for research administration. Participant characteristics The remaining participants were a convenience sample of women who were currently pregnant, recruited from a local antenatal care clinic. Interviewers approached women at the clinic and provided a brief explanation of the study. If the woman expressed interest, she was given the options of either reviewing the informed consent information and completing the interview after her clinic appointment in a private, adjacent room, or scheduling a more convenient time to return. Recruitment was designed around clinic flow and based on the limited availability of the interviewers. As such, an overall response rate was not calculated. As previously described [27], our objective in utilizing this sampling methodology was not to approximate a representative sample, but rather to surface and explore the range of issues and concrete considerations relevant to women who might be eligible to participate in studies while pregnant, that should inform discussions surrounding policy and best practices regarding the inclusion of pregnant women in clinical HIV prevention trials. Data for this analysis are based on 35 in-depth interviews conducted with reproductive-aged women at risk for HIV in Lilongwe, Malawi. In-depth interviews were utilized instead of focus groups because the topic—considerations regarding participation in HIV-related clinical trials during pregnancy—is highly personal and potentially sensitive, and we wanted to deeply explore women’s considerations about participating in such research. Interviews were conducted in Chichewa by two trained, bilingual, local social behavioral scientists both experienced in qualitative HIV research (TW and CZ), using a semi-structured guide between August 2016 and April 2017 [27]. Female interviewers were purposefully selected to encourage the comfort and candor of participants. Written informed consent was obtained prior to the interview, and women consented to being audio-recorded. Women also answered demographic questions and questions assessing their current pregnancy status, pregnancy history, and HIV testing/treatment history. Interviews lasted approximately 45–60 min. In line with recommendations by the National Health Science Research Committee of Malawi (NHSRC) at the time, participants were reimbursed 3500 Malawi Kwacha, the equivalent of $5 USD, for costs associated with participation (i.e., transportation). In the consent process, we described efforts to protect confidentiality, and assured participants that names and other identifying information would not be linked to their direct quotes in publications. The research was approved by the institutional review boards at the University of North Carolina (UNC) at Chapel Hill, Johns Hopkins University (JHU), and the National Health Science Research Committee of Malawi. Interview guide development was informed by a review of the scholarly literature on women’s participation in research during pregnancy, interviews with HIV investigators exploring barriers to and facilitators of including pregnant women in clinical trials [28], and consultations with researchers and healthcare providers in the U.S. and Malawi. The interview guide was developed in English, and then translated into Chichewa by TW and CZ. It was then used in preliminary interviews, and revised to enhance cultural appropriateness, clarity, and flow. As part of the interviews, we elicited women’s responses to the prospect of participating while pregnant in any of three hypothetical HIV prevention clinical trial vignettes, testing: (1) oral PrEP, (2) the vaginal ring, and (3) a randomized trial comparing the two (see Table 1). The use of succinct, standardized vignettes and subsequent probes allowed us to surface women’s initial receptiveness and considerations regarding participation within and across the trio of hypothetical HIV prevention research scenarios. The vignettes were read aloud to participants and consisted of a brief introductory overview of the purpose, design, participant requirements, and known safety data during pregnancy. Women were also provided a simple visual aid for each scenario. HIV biomedical prevention trial vignettes After each vignette was read, the interviewer would answer any questions the participant had about the scenario before proceeding. We then asked if women would participate in each vignette, and what was most important to them in making this decision. Additionally, participants were then told that, “Some people think about specific risks and benefits when they decide about participating in a study,” and asked if they thought about it this way. If participants responded affirmatively, we then probed specific risks and benefits to the baby and to the women themselves that they had considered. Interviews were audio recorded. After each interview, the interviewer wrote a summary and recorded her impressions. Trained, local bilingual research staff experienced in transcription and translation both transcribed the Chichewa audio recordings following a standardized protocol, and then translated the transcripts into English. The interviewer reviewed the Chichewa transcript for accuracy prior to translation, and again after they were translated into English. Additionally, the US-based Project Director (KS) reviewed the interview summaries and English transcripts as they were produced and provided feedback to the interviewers. English transcripts were uploaded into NVivo 11 for analysis. Codebook development was a collaborative process within the cross-cultural analytic team (KS, TW, EJ, and CZ) that began when the first 15 interviews were completed. Thematic analysis informed the analytic approach [29]. We familiarized ourselves with the data by reading and rereading the transcripts and summaries, and making notes of our impressions. Structural codes were first applied to organize the data by question and response. Content coding was then developed, with initial codes modified as we worked through the coding process with our research question in mind, and transcripts recoded as necessary. Throughout the coding process, the cross-cultural analysis team had extensive discussions about cultural and other meanings of responses. To enhance the cultural integrity and overall validity of the analysis, all transcripts were coded by at least one local researcher (TM, CZ). Additionally, to ensure intercoder reliability, 20% of the data were double coded, and any discrepancies were discussed until consensus was reached through re-coding or revising our understandings of the codes. With NVivo 11 software, we extracted the text for the interview sections of interest, and utilized data display matrices to make comparisons within and across respondents and identify thematically and conceptually overarching themes. Sub-themes were grouped into themes based on thematic similarities, and the dataset was analyzed for the prevalence and breadth of identified themes. Summaries of each theme including exemplary quotes are presented. Data saturation was assessed and confirmed as coding progressed and no new themes were found in subsequent transcripts [30]. Demographics were self-reported by participants. Of note, the cultural concept of marriage in Malawi extends beyond the legal definition and includes co-habitating couples jointly raising children. Methods are also described in detail elsewhere [27].

AI Digest

Study Justification:

The study aimed to explore the views of Malawian women regarding participation in HIV prevention clinical trials during pregnancy. This research is important because there is a need to expand the biomedical HIV prevention evidence base for pregnant women. Understanding women’s perspectives on participating in such trials and initiating pre-exposure prophylaxis (PrEP) while pregnant is crucial for informing policy and best practices to ensure responsible access to evidence-based interventions for this population.

Highlights:

– The majority of women expressed a strong interest in participating in biomedical HIV prevention research during pregnancy.
– Women’s motivation for participation was driven by a desire to protect themselves and their offspring from HIV.
– Participants highlighted the health benefits of participation, including HIV protection, access to testing/treatment, and ancillary care.
– Perceived risks of the trial were generally low, while potential maternal and fetal health risks were raised by women who were uninterested in participating.
– Power dynamics with partners, challenges of justifying prevention use, and social networks were factors influencing participation decisions.

Recommendations for Lay Reader and Policy Maker:

1. Based on the study findings, it is recommended to continue expanding access to biomedical HIV prevention research during pregnancy.
2. Policy makers should prioritize the inclusion of pregnant women in clinical trials to ensure their health and the health of their offspring are protected.
3. Efforts should be made to address the concerns raised by women who are uninterested in participating, particularly regarding maternal and fetal health risks.
4. Education and awareness campaigns should be conducted to inform women about the benefits and risks of participating in HIV prevention trials during pregnancy.
5. Supportive measures should be put in place to address power dynamics with partners and challenges of justifying prevention use.

Key Role Players:

1. Researchers and scientists involved in HIV prevention research.
2. Healthcare providers and clinicians specializing in reproductive health and HIV/AIDS.
3. Policy makers and government officials responsible for healthcare and research regulations.
4. Community leaders and organizations working on women’s health and HIV prevention.
5. Non-governmental organizations (NGOs) involved in HIV/AIDS prevention and advocacy.

Cost Items for Planning Recommendations:

1. Research funding for conducting clinical trials and collecting data.
2. Training and capacity-building programs for healthcare providers and researchers.
3. Development and implementation of education and awareness campaigns.
4. Support services for participants, including transportation and reimbursement for participation costs.
5. Monitoring and evaluation of the implementation of research policies and practices.
Please note that the cost items provided are general categories and not actual cost estimates. The specific budget items would depend on the scale and scope of the interventions and programs implemented.

Força da prova

The strength of evidence for this abstract is 8 out of 10.
The evidence in the abstract is strong because it presents the findings of a qualitative study conducted with a diverse sample of reproductive-aged women in Malawi. The study utilized semi-structured interviews, thematic analysis, and triangulation of data to explore women’s perspectives on participating in HIV prevention clinical trials during pregnancy. The study provides detailed information on the participants, data collection methods, and analysis process. However, to improve the evidence, it would be helpful to include information on the sample size and demographic characteristics of the participants, as well as any limitations of the study.

Resumo

The data for this analysis were collected in partnership with UNC Project Malawi and as part of a larger project, Pregnancy and HIV/AIDS: Seeking Equitable Study (PHASES). We conducted qualitative, in-depth interviews using a semi-structured guide to assess the views of women who might be eligible to participate in HIV research during pregnancy about (1) their experiences with research; (2) selected rules governing the intersection of research and reproduction; and (3) their responses to theoretical vignettes describing research during pregnancy. The latter are reported here. Participants included in this analysis were all HIV-negative, and purposively sampled to capture a range of experience with research during pregnancy. UNC Project Malawi in Lilongwe is a study site for U.S. National Institute of Allergy and Infectious Diseases (NIAID) HIV/AIDS Clinical Trials Network studies, many of which involve women of reproductive age. Just over half of the sample (see Table 2) were either: (1) women who had previously participated in a biomedical HIV prevention trial during pregnancy, or (2) women who were denied enrollment in a biomedical HIV prevention trial due to pregnancy; women meeting either criterion are described here as “research experienced”. Research experienced participants were identified by Malawi based research outreach staff through existing trial participation records at UNC Project Malawi. For this purposively selected research experienced subsample, current pregnancy status was not an eligibility requirement. Outreach staff contacted the women by phone, provided a brief description of the study, and invited them to participate. Those who indicated interest were scheduled for an interview appointment in a private office used for research administration. Participant characteristics The remaining participants were a convenience sample of women who were currently pregnant, recruited from a local antenatal care clinic. Interviewers approached women at the clinic and provided a brief explanation of the study. If the woman expressed interest, she was given the options of either reviewing the informed consent information and completing the interview after her clinic appointment in a private, adjacent room, or scheduling a more convenient time to return. Recruitment was designed around clinic flow and based on the limited availability of the interviewers. As such, an overall response rate was not calculated. As previously described [27], our objective in utilizing this sampling methodology was not to approximate a representative sample, but rather to surface and explore the range of issues and concrete considerations relevant to women who might be eligible to participate in studies while pregnant, that should inform discussions surrounding policy and best practices regarding the inclusion of pregnant women in clinical HIV prevention trials. Data for this analysis are based on 35 in-depth interviews conducted with reproductive-aged women at risk for HIV in Lilongwe, Malawi. In-depth interviews were utilized instead of focus groups because the topic—considerations regarding participation in HIV-related clinical trials during pregnancy—is highly personal and potentially sensitive, and we wanted to deeply explore women’s considerations about participating in such research. Interviews were conducted in Chichewa by two trained, bilingual, local social behavioral scientists both experienced in qualitative HIV research (TW and CZ), using a semi-structured guide between August 2016 and April 2017 [27]. Female interviewers were purposefully selected to encourage the comfort and candor of participants. Written informed consent was obtained prior to the interview, and women consented to being audio-recorded. Women also answered demographic questions and questions assessing their current pregnancy status, pregnancy history, and HIV testing/treatment history. Interviews lasted approximately 45–60 min. In line with recommendations by the National Health Science Research Committee of Malawi (NHSRC) at the time, participants were reimbursed 3500 Malawi Kwacha, the equivalent of $5 USD, for costs associated with participation (i.e., transportation). In the consent process, we described efforts to protect confidentiality, and assured participants that names and other identifying information would not be linked to their direct quotes in publications. The research was approved by the institutional review boards at the University of North Carolina (UNC) at Chapel Hill, Johns Hopkins University (JHU), and the National Health Science Research Committee of Malawi. Interview guide development was informed by a review of the scholarly literature on women’s participation in research during pregnancy, interviews with HIV investigators exploring barriers to and facilitators of including pregnant women in clinical trials [28], and consultations with researchers and healthcare providers in the U.S. and Malawi. The interview guide was developed in English, and then translated into Chichewa by TW and CZ. It was then used in preliminary interviews, and revised to enhance cultural appropriateness, clarity, and flow. As part of the interviews, we elicited women’s responses to the prospect of participating while pregnant in any of three hypothetical HIV prevention clinical trial vignettes, testing: (1) oral PrEP, (2) the vaginal ring, and (3) a randomized trial comparing the two (see Table 1). The use of succinct, standardized vignettes and subsequent probes allowed us to surface women’s initial receptiveness and considerations regarding participation within and across the trio of hypothetical HIV prevention research scenarios. The vignettes were read aloud to participants and consisted of a brief introductory overview of the purpose, design, participant requirements, and known safety data during pregnancy. Women were also provided a simple visual aid for each scenario. HIV biomedical prevention trial vignettes After each vignette was read, the interviewer would answer any questions the participant had about the scenario before proceeding. We then asked if women would participate in each vignette, and what was most important to them in making this decision. Additionally, participants were then told that, “Some people think about specific risks and benefits when they decide about participating in a study,” and asked if they thought about it this way. If participants responded affirmatively, we then probed specific risks and benefits to the baby and to the women themselves that they had considered. Interviews were audio recorded. After each interview, the interviewer wrote a summary and recorded her impressions. Trained, local bilingual research staff experienced in transcription and translation both transcribed the Chichewa audio recordings following a standardized protocol, and then translated the transcripts into English. The interviewer reviewed the Chichewa transcript for accuracy prior to translation, and again after they were translated into English. Additionally, the US-based Project Director (KS) reviewed the interview summaries and English transcripts as they were produced and provided feedback to the interviewers. English transcripts were uploaded into NVivo 11 for analysis. Codebook development was a collaborative process within the cross-cultural analytic team (KS, TW, EJ, and CZ) that began when the first 15 interviews were completed. Thematic analysis informed the analytic approach [29]. We familiarized ourselves with the data by reading and rereading the transcripts and summaries, and making notes of our impressions. Structural codes were first applied to organize the data by question and response. Content coding was then developed, with initial codes modified as we worked through the coding process with our research question in mind, and transcripts recoded as necessary. Throughout the coding process, the cross-cultural analysis team had extensive discussions about cultural and other meanings of responses. To enhance the cultural integrity and overall validity of the analysis, all transcripts were coded by at least one local researcher (TM, CZ). Additionally, to ensure intercoder reliability, 20% of the data were double coded, and any discrepancies were discussed until consensus was reached through re-coding or revising our understandings of the codes. With NVivo 11 software, we extracted the text for the interview sections of interest, and utilized data display matrices to make comparisons within and across respondents and identify thematically and conceptually overarching themes. Sub-themes were grouped into themes based on thematic similarities, and the dataset was analyzed for the prevalence and breadth of identified themes. Summaries of each theme including exemplary quotes are presented. Data saturation was assessed and confirmed as coding progressed and no new themes were found in subsequent transcripts [30]. Demographics were self-reported by participants. Of note, the cultural concept of marriage in Malawi extends beyond the legal definition and includes co-habitating couples jointly raising children. Methods are also described in detail elsewhere [27].

Materiais

N/A

Inovações

Based on the provided information, here are some potential innovations that can be used to improve access to maternal health:

1. Mobile Health (mHealth) Solutions: Develop mobile applications or text messaging services to provide pregnant women with important health information, reminders for prenatal visits, and access to telemedicine consultations.

2. Community Health Workers: Train and deploy community health workers to provide education, counseling, and support to pregnant women in remote or underserved areas. These workers can also help with referrals and follow-up care.

3. Telemedicine: Establish telemedicine platforms that allow pregnant women to consult with healthcare providers remotely, reducing the need for travel and improving access to specialized care.

4. Maternal Health Vouchers: Implement voucher programs that provide pregnant women with financial assistance to cover the costs of prenatal care, delivery, and postnatal care. This can help overcome financial barriers to accessing maternal health services.

5. Transportation Solutions: Develop transportation initiatives, such as mobile clinics or transportation subsidies, to ensure that pregnant women can easily reach healthcare facilities for prenatal visits and emergency obstetric care.

6. Maternal Health Information Systems: Implement electronic health records and data management systems specifically designed for maternal health. This can improve coordination of care, enable better monitoring of maternal health outcomes, and facilitate research and policy development.

7. Maternal Health Education Programs: Develop comprehensive educational programs that target pregnant women and their families, providing information on prenatal care, nutrition, breastfeeding, and birth preparedness. These programs can be delivered through community workshops, mobile apps, or online platforms.

8. Public-Private Partnerships: Foster collaborations between public health agencies, private healthcare providers, and non-profit organizations to improve access to maternal health services. This can involve sharing resources, expertise, and infrastructure to reach more pregnant women and provide comprehensive care.

9. Maternal Health Financing Models: Explore innovative financing models, such as social health insurance or microinsurance, to ensure that pregnant women have access to affordable and quality maternal health services.

10. Maternal Health Task Forces: Establish multi-stakeholder task forces or committees dedicated to improving maternal health outcomes. These groups can coordinate efforts, advocate for policy changes, and monitor progress towards reducing maternal mortality and improving access to care.

It is important to note that the specific context and needs of the target population should be considered when implementing these innovations.

AI Innovations Description

The recommendation to improve access to maternal health based on the described study is to prioritize the inclusion of pregnant women in biomedical HIV prevention research. The study found that the majority of participants expressed a strong interest in participating in such trials, motivated by a desire to protect themselves and their offspring. This indicates that pregnant women are willing to engage in research that can provide them with HIV protection, testing, treatment, and ancillary care.

To develop this recommendation into an innovation, the following steps can be taken:

1. Collaboration: Foster collaboration between researchers, healthcare providers, and policymakers to develop guidelines and protocols that prioritize the inclusion of pregnant women in biomedical HIV prevention research. This collaboration should involve local stakeholders, such as community leaders and organizations, to ensure cultural appropriateness and acceptance.

2. Education and Awareness: Conduct educational campaigns to raise awareness among pregnant women about the importance of participating in biomedical HIV prevention research. This can include providing information about the potential benefits of participation, addressing misconceptions or concerns, and highlighting the role of research in improving maternal health outcomes.

3. Training and Capacity Building: Provide training and capacity building initiatives for healthcare providers and researchers to ensure they have the necessary knowledge and skills to conduct biomedical HIV prevention research during pregnancy. This can include training on ethical considerations, informed consent processes, and the safe administration of prevention products.

4. Access to Prevention Products: Ensure that pregnant women have access to a range of HIV prevention products, such as oral PrEP and vaginal rings, through healthcare facilities and research sites. This can involve working with pharmaceutical companies, governments, and international organizations to prioritize the availability and affordability of these products for pregnant women.

5. Supportive Care: Implement comprehensive care packages that address the specific needs of pregnant women participating in biomedical HIV prevention research. This can include providing counseling services, addressing social and economic barriers to participation, and offering support for adherence to prevention products.

By implementing these recommendations, it is possible to develop an innovation that improves access to maternal health by including pregnant women in biomedical HIV prevention research. This innovation can contribute to the evidence base and inform policies and practices aimed at protecting the health of pregnant women and their offspring.

AI Innovations Methodology

Based on the provided information, it seems that the study focused on understanding the views of Malawian women regarding participation in HIV prevention clinical trials during pregnancy. The study utilized qualitative research methods, specifically semi-structured interviews, to gather data from 35 reproductive-aged women in Malawi. The interviews were conducted in the local language, Chichewa, and were audio-recorded, transcribed, translated, and coded using NVivo 11 software.

To simulate the impact of recommendations on improving access to maternal health, a potential methodology could involve the following steps:

1. Identify the recommendations: Based on the findings of the study and other relevant research, identify specific recommendations that could improve access to maternal health. These recommendations could include interventions, policies, or strategies aimed at addressing barriers to accessing maternal health services.

2. Define indicators: Determine the indicators that will be used to measure the impact of the recommendations on improving access to maternal health. These indicators could include metrics such as the number of women accessing prenatal care, the percentage of women receiving skilled birth attendance, or the reduction in maternal mortality rates.

3. Collect baseline data: Collect baseline data on the selected indicators to establish a starting point for measuring the impact of the recommendations. This could involve gathering data from existing sources such as health records, surveys, or interviews with healthcare providers.

4. Implement the recommendations: Implement the identified recommendations to improve access to maternal health. This could involve implementing new programs or interventions, changing policies or guidelines, or strengthening existing healthcare systems.

5. Monitor and evaluate: Continuously monitor and evaluate the impact of the implemented recommendations on the selected indicators. This could involve collecting data at regular intervals to track changes over time.

6. Analyze the data: Analyze the collected data to assess the impact of the recommendations on improving access to maternal health. This could involve statistical analysis, comparing the baseline data with the data collected after implementing the recommendations.

7. Draw conclusions and make recommendations: Based on the analysis of the data, draw conclusions about the effectiveness of the recommendations in improving access to maternal health. Make recommendations for further improvements or adjustments to the implemented interventions or policies.

It is important to note that the specific methodology for simulating the impact of recommendations on improving access to maternal health may vary depending on the context, available resources, and research objectives. The methodology described above provides a general framework that can be adapted and customized to suit the specific needs of the study.

Autores & Coautores

Statistics:

Citations: 4

Authors: 9

Identifiers:

DOI: 10.1186/s12981-020-00271-6

Research Areas:

Community Interventions, Health System and Policy, Infectious Diseases, Maternal Access, Maternal and Child Health, Quality of Care, Sexual and Reproductive Health, Social Determinants

Study Countries:

Malawi

Study Design:

Cross Sectional Study

Study Approach:

Qualitative

Participants Gender:

Female

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