Cost-effectiveness of World Health Organization 2010 guidelines for prevention of mother-to-child HIV transmission in Zimbabwe

Clinical Infectious Diseases, Volume 56, No. 3, Year 2013

Ukuhunyushwa

Background. In 2010, the World Health Organization (WHO) released revised guidelines for prevention of mother-to-child human immunodeficiency virus (HIV) transmission (PMTCT). We projected clinical impacts, costs, and cost-effectiveness of WHO-recommended PMTCT strategies in Zimbabwe.Methods. We used Zimbabwean data in a validated computer model to simulate a cohort of pregnant, HIV-infected women (mean age, 24 years; mean CD4 count, 451 cells/L; subsequent 18 months of breastfeeding). We simulated guideline-concordant care for 4 PMTCT regimens: single-dose nevirapine (sdNVP); WHO-recommended Option A, WHO-recommended Option B, and Option B+ (lifelong maternal 3-drug antiretroviral therapy regardless of CD4). Outcomes included maternal and infant life expectancy (LE) and lifetime healthcare costs (2008 US dollars [USD]). Incremental cost-effectiveness ratios (ICERs, in USD per year of life saved [YLS]) were calculated from combined (maternal + infant) discounted costs and LE.Results. Replacing sdNVP with Option A increased combined maternal and infant LE from 36.97 to 37.89 years and would reduce lifetime costs from $5760 to $5710 per mother-infant pair. Compared with Option A, Option B further improved LE (38.32 years), and saved money within 4 years after delivery ($5630 per mother-infant pair). Option B+ (LE, 39.04 years; lifetime cost, $6620 per mother-infant pair) improved maternal and infant health, with an ICER of $1370 per YLS compared with Option B.Conclusions. Replacing sdNVP with Option A or Option B will improve maternal and infant outcomes and save money; Option B increases health benefits and decreases costs compared with Option A. Option B+ further improves maternal outcomes, with an ICER (compared with Option B) similar to many current HIV-related healthcare interventions. © 2012 The Author 2012. We used 3 validated, linked computer models for this analysis (Figure (Figure1):1): (1) a model of a single pregnancy and delivery (the mother-to-child HIV transmission [MTCT] model [10]); (2) the Cost-effectiveness of Preventing AIDS Complications (CEPAC) model of HIV infection and mortality among breastfed infants (the CEPAC infant model [13, 14]); and (3) the CEPAC-International model of HIV disease progression among postpartum women (the CEPAC adult model [11, 12, 15]). Clinical outcomes of the linked models included infant HIV infection risk at weaning, maternal life expectancy (LE) from delivery, and infant LE from birth. Economic outcomes, from the healthcare system perspective, included ANC costs (through delivery), maternal HIV-related healthcare costs, and infant healthcare costs. Model structure. Three linked models were used for this analysis, as described in the Methods, as well as in the Supplementary Appendix and previous work [10, 14, 15]. The mother-to-child human immunodeficiency virus transmission model includes events during pregnancy and delivery (left panel; Supplementary Figure 1). The Cost-effectiveness of Preventing AIDS Complications (CEPAC) adult model includes events occurring among mothers after delivery (bottom right panel; Supplementary Figure 2A), and the CEPAC infant model includes events for infants after birth (top right panel; Supplementary Figure 2B). Linkages between the models allow a combined analysis in which each woman–infant pair is simulated together from the time of first presentation at antenatal care through pregnancy and delivery, and then each woman and infant are simulated separately throughout their lifetimes. Abbreviations: ANC, antenatal care; ART, 2-drug antiretroviral therapy; ARVs, antiretroviral medications; HIV, human immunodeficiency virus; OI, opportunistic infection; PMTCT, prevention of mother-to-child HIV transmission; sdNVP, single-dose nevirapine. Incremental cost-effectiveness ratios (ICERs), in US dollars per year of life saved (YLS), were calculated from combined projected lifetime healthcare costs (antenatal + maternal + infant) and combined projected life expectancy (maternal + infant) [16], discounted at 3% per year. We used 2 criteria to interpret cost-effectiveness. First, following WHO guidance, an intervention was considered cost-effective if its ICER compared with the next least-expensive alternative was <3 times the 2008 Zimbabwe per capita gross domestic product, or 3 × $400 = $1200 per YLS [17, 18]. Second, we compared results with the recently reported range of ICERs for ART-related interventions in developing countries ($550–$5200 per YLS) [19]. This work was approved by the Partners Healthcare Institutional Review Board, Boston, Massachusetts. The linked models were used to simulate a cohort of pregnant, HIV-infected women in Zimbabwe and their infants. We examined 5 PMTCT regimens: (1) no antenatal ARVs (comparator), (2) sdNVP, (3) WHO Option A, (4) WHO Option B, and (5) Option B+ (Supplementary Table 1). Women were modeled to present to care at 24–28 weeks’ gestation and to breastfeed for 18 months, based on Zimbabwean data [20, 21], with ARV prophylaxis (Options A, B, and B+ ) continued throughout breastfeeding. To demonstrate the impact of guideline-concordant care, all women in the base-case analyses were assumed to be identified as HIV-infected at their first ANC visit. With no ARVs, women received no antiretroviral medications during pregnancy. With sdNVP, women initiated ART in pregnancy if clinical assessment indicated WHO stage 3–4 disease; CD4 testing was not included, reflecting its limited availability in the sdNVP-based National PMTCT Program in 2009. With Options A and B, women received ART during pregnancy if eligible by either CD4 or clinical criteria, and with Option B+, all women received lifelong ART. With all modeled regimens, women who linked to postnatal HIV care were assumed to undergo clinical and CD4 assessment at 6 weeks postpartum and to initiate ART if eligible, regardless of antenatal regimen received. In the base case, we assumed 100% adherence to PMTCT regimens (initiated at 30 weeks’ gestational age), 100% linkage to postnatal care for mothers and infants, and 100% retention in care and ART availability for women and infants meeting WHO ART initiation criteria [22, 23]. In sensitivity analyses, to reflect real-world programs, we examined reduced access to antenatal and postnatal care. The 3 simulation models are described in detail in the Supplementary Appendix and in previous publications [10, 14, 15]. The models were linked so that each mother–infant pair was simulated together from the time of first presentation at ANC through delivery (the MTCT model), and then each woman and infant were simulated separately over their lifetimes after delivery (the CEPAC adult and infant models), as in Figure Figure11 and Supplementary Figures 1 and 2. Based on Zimbabwean data, mean age at first ANC visit was 24 years [21]; mean CD4 count was 451 cells/µL (36% of women with CD4 count ≤350 cells/µL) [24]. Because detailed data to inform monthly risks of opportunistic infections (OIs) and HIV-related death in the absence of ART were not available from Zimbabwe, we derived these data from a cohort in South Africa (Supplementary Table 2) [25]. Details of ART initiation and switching, as well as CD4 and HIV RNA changes on ART, are provided in the Supplementary Appendix. Risks of MTCT during pregnancy and breastfeeding were calculated from PMTCT studies among breastfeeding populations in Africa, leading to estimates similar to those derived by the Joint United Nations Programme on HIV/AIDS (Supplementary Appendix) [10, 26]. Data and assumptions to inform infant mortality rates and LE values are shown in Table Table11 and detailed in the Supplementary Appendix. Selected Model Input Parameters See Supplementary Table 2 for complete list of parameters. Abbreviations: 3TC, lamivudine; ANC, antenatal care; ART, antiretroviral therapy; ARV, antiretroviral medications; d4T, stavudine; EBF, exclusive breastfeeding (in first 6 months of life, followed by MBF); EFV, efavirenz; FTC, emtricabine; HIV, human immunodeficiency virus; LPV/r, lopinavir/ritonavir; MACS, Multicenter AIDS Cohort Study; MBF, mixed breastfeeding; MOHCW, Zimbabwe Ministry of Health and Child Welfare; NA, not applicable; NVP, nevirapine; PTMCT, prevention of mother-to-child HIV transmission; SD, standard deviation; sdNVP, single-dose nevirapine; TDF, tenofovir; WHO, World Health Organization; ZDV, zidovudine. a ART eligibility was defined as CD4 count of ≤350 cells/µL or WHO stage 3–4 disease. b PMTCT uptake was defined as proportion of HIV-infected, pregnant women accessing PMTCT services by the time of delivery. See Supplementary Appendix text and Supplementary Table 2 for details. c Two months of antentatal drug are assumed in all regimens for the base-case analysis, based on median gestational age at booking in Zimbabwe of 30 weeks. d Total care costs for mothers and infants were calculated by multiplying resource utilization (number of outpatient visits and inpatient days) by an average of WHO-CHOICE estimates of costs for these encounters in 7 sub–Saharan African countries [28]. See Supplementary Appendix for details. e See Supplementary Table 2 for description of assumptions of outpatient healthcare resource utilization. Monthly medication costs were from the Clinton Healthcare Access Initiative [27]. Costs of clinical care were determined by estimating resource utilization (number of inpatient days and outpatient visits) for specified health conditions, then multiplying by the estimated costs of these healthcare encounters in Zimbabwe (Table (Table11 and Supplementary Appendix) [28]. For children aged >18 months, monthly utilization estimates (stratified by HIV and ART status) were multiplied by LE to estimate lifetime healthcare costs. Model-derived risks of MTCT, infant mortality, and postpartum maternal OIs were validated against published data, reported previously with extensive sensitivity analyses [10, 14]. For this study, we conducted univariate and multivariate sensitivity analyses on key PMTCT, pediatric, maternal, and cost parameters. We examined the impact of reported rates of PMTCT uptake, defined as the proportion of HIV-infected women receiving PMTCT services and ARVs by delivery (56%, estimated for Zimbabwe in 2009; 80%, the 2009 WHO target goal; 90%, the 2011 WHO target goal; and 95%, reported in neighboring Botswana in 2011) [5, 8, 29]. We varied the availability of CD4 assays from 25% to 100% in Options A, B, and B+; when CD4 count was unavailable in Option A, women were assumed to initiate ART only for WHO stage 3–4 disease. We also examined the impact of reduced pediatric ART availability (36%, estimated for Zimbabwe in 2009) [5] and of reported rates of maternal loss to follow-up (LTFU) from postnatal HIV care (Table (Table1)1) [30–32]. We defined a lowest-MTCT risk scenario, using the lowest published risks (best reported effectiveness/efficacy) for each modeled regimen (Table (Table1);1); a highest-MTCT risk scenario, combining the highest published risks for each regimen; and a scenario assuming equal MTCT risks with Options A and B. We also used 4 assumptions about LE for HIV-exposed and HIV-infected infants: (1) a high pediatric LE scenario, using the upper bound estimates shown in Table Table1,1, (2) a low pediatric LE scenario, using the lower bound estimates, (3) a largest difference scenario (lowest estimates for HIV-infected children; highest estimates for HIV-uninfected children), and (4) a smallest difference scenario (highest estimates for HIV-infected children; lowest estimates for uninfected children). Finally, we investigated potential maternal health impacts of Option B and B+ in 2 ways. First, we varied the efficacy of first-line ART when resumed after ART interruption, reflecting potential interruption-associated drug resistance. Next, we examined the impact of “treatment fatigue” for women who begin ART with CD4 count >350 cells/µL solely for PMTCT, modeled as (1) an increased risk of virologic failure >6 months after ART initiation or (2) a reduction in second-line ART efficacy. Because estimated costs of healthcare in Zimbabwe are markedly lower than in surrounding countries [28], we repeated the analysis using costs from South Africa (Supplementary Table 2) [33]. In the base case, we conservatively assigned lifelong costs of NVP-based ART to HIV-infected infants; in sensitivity analyses, as an upper bound on pediatric ART costs, we assigned the costs of lifelong lopinavir/ritonavir-based ART to sdNVP-exposed, HIV-infected children. Finally, the nondrug costs of providing 3-drug ARV regimens instead of zidovudine alone (e.g., personnel, laboratory costs) have not been reported; we also examined the impact of such implementation costs in the antenatal period.

I-AI Digest

Study Justification:

The study aimed to evaluate the cost-effectiveness of the World Health Organization (WHO) 2010 guidelines for the prevention of mother-to-child HIV transmission (PMTCT) in Zimbabwe. The study projected the clinical impacts, costs, and cost-effectiveness of the WHO-recommended PMTCT strategies in Zimbabwe.

Highlights:

– Replacing single-dose nevirapine (sdNVP) with WHO Option A increased the life expectancy of both mothers and infants and reduced lifetime costs per mother-infant pair.
– WHO Option B further improved life expectancy and saved money within 4 years after delivery compared to Option A.
– Option B+ improved maternal and infant health and had a cost-effectiveness ratio of $1370 per year of life saved compared to Option B.

Recommendations for a Lay Reader:

– Replacing sdNVP with Option A or Option B will improve the health outcomes of mothers and infants and save money.
– Option B is more beneficial and cost-effective compared to Option A.
– Option B+ provides further improvements in maternal outcomes and is cost-effective compared to Option B.

Recommendations for a Policy Maker:

– Implementing WHO Option A or Option B for PMTCT in Zimbabwe will improve maternal and infant outcomes and save money.
– Option B is more beneficial and cost-effective compared to Option A.
– Consider implementing Option B+ to further improve maternal outcomes, as it is cost-effective compared to Option B.

Key Role Players:

– Ministry of Health and Child Welfare (MOHCW)
– Healthcare providers
– HIV/AIDS program managers
– Policy makers
– Researchers and scientists

Cost Items to Include in Planning the Recommendations:

– Antenatal care costs
– Maternal HIV-related healthcare costs
– Infant healthcare costs
– Costs of antiretroviral medications
– Costs of clinical care (outpatient visits and inpatient days)
– Costs of laboratory tests
– Personnel costs
– Implementation costs of 3-drug antiretroviral regimens
Note: The provided information is based on the description and findings of the study.

Amandla Obufakazi

The strength of evidence for this abstract is 8 out of 10.
The evidence in the abstract is strong because it is based on a validated computer model using Zimbabwean data. The study examines multiple PMTCT regimens and calculates clinical impacts, costs, and cost-effectiveness. The results show that replacing sdNVP with Option A or Option B improves maternal and infant outcomes and saves money. Option B+ further improves maternal outcomes. However, to improve the evidence, the study could include more real-world data and consider the impact of reduced access to antenatal and postnatal care.

Abstract

We used 3 validated, linked computer models for this analysis (Figure (Figure1):1): (1) a model of a single pregnancy and delivery (the mother-to-child HIV transmission [MTCT] model [10]); (2) the Cost-effectiveness of Preventing AIDS Complications (CEPAC) model of HIV infection and mortality among breastfed infants (the CEPAC infant model [13, 14]); and (3) the CEPAC-International model of HIV disease progression among postpartum women (the CEPAC adult model [11, 12, 15]). Clinical outcomes of the linked models included infant HIV infection risk at weaning, maternal life expectancy (LE) from delivery, and infant LE from birth. Economic outcomes, from the healthcare system perspective, included ANC costs (through delivery), maternal HIV-related healthcare costs, and infant healthcare costs. Model structure. Three linked models were used for this analysis, as described in the Methods, as well as in the Supplementary Appendix and previous work [10, 14, 15]. The mother-to-child human immunodeficiency virus transmission model includes events during pregnancy and delivery (left panel; Supplementary Figure 1). The Cost-effectiveness of Preventing AIDS Complications (CEPAC) adult model includes events occurring among mothers after delivery (bottom right panel; Supplementary Figure 2A), and the CEPAC infant model includes events for infants after birth (top right panel; Supplementary Figure 2B). Linkages between the models allow a combined analysis in which each woman–infant pair is simulated together from the time of first presentation at antenatal care through pregnancy and delivery, and then each woman and infant are simulated separately throughout their lifetimes. Abbreviations: ANC, antenatal care; ART, 2-drug antiretroviral therapy; ARVs, antiretroviral medications; HIV, human immunodeficiency virus; OI, opportunistic infection; PMTCT, prevention of mother-to-child HIV transmission; sdNVP, single-dose nevirapine. Incremental cost-effectiveness ratios (ICERs), in US dollars per year of life saved (YLS), were calculated from combined projected lifetime healthcare costs (antenatal + maternal + infant) and combined projected life expectancy (maternal + infant) [16], discounted at 3% per year. We used 2 criteria to interpret cost-effectiveness. First, following WHO guidance, an intervention was considered cost-effective if its ICER compared with the next least-expensive alternative was 18 months, monthly utilization estimates (stratified by HIV and ART status) were multiplied by LE to estimate lifetime healthcare costs. Model-derived risks of MTCT, infant mortality, and postpartum maternal OIs were validated against published data, reported previously with extensive sensitivity analyses [10, 14]. For this study, we conducted univariate and multivariate sensitivity analyses on key PMTCT, pediatric, maternal, and cost parameters. We examined the impact of reported rates of PMTCT uptake, defined as the proportion of HIV-infected women receiving PMTCT services and ARVs by delivery (56%, estimated for Zimbabwe in 2009; 80%, the 2009 WHO target goal; 90%, the 2011 WHO target goal; and 95%, reported in neighboring Botswana in 2011) [5, 8, 29]. We varied the availability of CD4 assays from 25% to 100% in Options A, B, and B+; when CD4 count was unavailable in Option A, women were assumed to initiate ART only for WHO stage 3–4 disease. We also examined the impact of reduced pediatric ART availability (36%, estimated for Zimbabwe in 2009) [5] and of reported rates of maternal loss to follow-up (LTFU) from postnatal HIV care (Table (Table1)1) [30–32]. We defined a lowest-MTCT risk scenario, using the lowest published risks (best reported effectiveness/efficacy) for each modeled regimen (Table (Table1);1); a highest-MTCT risk scenario, combining the highest published risks for each regimen; and a scenario assuming equal MTCT risks with Options A and B. We also used 4 assumptions about LE for HIV-exposed and HIV-infected infants: (1) a high pediatric LE scenario, using the upper bound estimates shown in Table Table1,1, (2) a low pediatric LE scenario, using the lower bound estimates, (3) a largest difference scenario (lowest estimates for HIV-infected children; highest estimates for HIV-uninfected children), and (4) a smallest difference scenario (highest estimates for HIV-infected children; lowest estimates for uninfected children). Finally, we investigated potential maternal health impacts of Option B and B+ in 2 ways. First, we varied the efficacy of first-line ART when resumed after ART interruption, reflecting potential interruption-associated drug resistance. Next, we examined the impact of “treatment fatigue” for women who begin ART with CD4 count >350 cells/µL solely for PMTCT, modeled as (1) an increased risk of virologic failure >6 months after ART initiation or (2) a reduction in second-line ART efficacy. Because estimated costs of healthcare in Zimbabwe are markedly lower than in surrounding countries [28], we repeated the analysis using costs from South Africa (Supplementary Table 2) [33]. In the base case, we conservatively assigned lifelong costs of NVP-based ART to HIV-infected infants; in sensitivity analyses, as an upper bound on pediatric ART costs, we assigned the costs of lifelong lopinavir/ritonavir-based ART to sdNVP-exposed, HIV-infected children. Finally, the nondrug costs of providing 3-drug ARV regimens instead of zidovudine alone (e.g., personnel, laboratory costs) have not been reported; we also examined the impact of such implementation costs in the antenatal period.

Izinto zokwakha

Emisha

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 SMS-based systems to provide pregnant women with information on antenatal care, HIV prevention, and PMTCT guidelines. These solutions can also be used to send reminders for appointments and medication adherence.

2. Telemedicine: Implement telemedicine services to provide remote consultations and follow-up care for pregnant women, especially in rural areas where access to healthcare facilities is limited. This can help improve access to specialized care and reduce the need for travel.

3. Community Health Workers: Train and deploy community health workers to provide education, counseling, and support to pregnant women in their communities. These workers can help increase awareness about maternal health, promote early antenatal care, and facilitate access to PMTCT services.

4. Task Shifting: Expand the roles and responsibilities of healthcare providers, such as nurses and midwives, to perform certain tasks traditionally done by doctors. This can help alleviate the shortage of healthcare professionals and improve access to maternal health services.

5. Integration of Services: Integrate maternal health services with other healthcare programs, such as family planning and HIV care, to provide comprehensive care for women. This can help streamline service delivery and ensure continuity of care.

6. Quality Improvement Initiatives: Implement quality improvement initiatives to enhance the delivery of maternal health services. This can involve training healthcare providers, improving infrastructure and equipment, and strengthening monitoring and evaluation systems.

7. Public-Private Partnerships: Foster collaborations between the public and private sectors to improve access to maternal health services. This can involve leveraging the resources and expertise of private healthcare providers, pharmaceutical companies, and technology companies.

8. Financial Innovations: Develop innovative financing mechanisms, such as health insurance schemes or microfinance programs, to make maternal health services more affordable and accessible to women, especially those from low-income backgrounds.

9. Community Engagement: Engage communities in the planning, implementation, and monitoring of maternal health programs. This can help increase community ownership, address cultural and social barriers, and ensure that services are tailored to the specific needs of the population.

10. Research and Innovation: Invest in research and innovation to continuously improve maternal health services. This can involve conducting studies to identify barriers and solutions, testing new interventions, and adapting evidence-based practices from other settings.

It is important to note that these recommendations are general and may need to be adapted to the specific context and resources available in Zimbabwe.

AI Innovations Description

The recommendation that can be used to develop an innovation to improve access to maternal health is to implement the World Health Organization (WHO) 2010 guidelines for prevention of mother-to-child HIV transmission (PMTCT) in Zimbabwe. The study mentioned in the description found that following the WHO-recommended PMTCT strategies, such as Option A, Option B, and Option B+, can improve maternal and infant outcomes and save money.

Option A involves providing antiretroviral therapy (ART) during pregnancy to eligible women based on CD4 count or clinical criteria. Option B includes lifelong ART for all pregnant women, regardless of CD4 count. Option B+ is similar to Option B but also includes lifelong ART for women after delivery.

By implementing these guidelines, the study projected that maternal and infant life expectancy would increase, and lifetime healthcare costs would decrease. Option B was found to be more cost-effective compared to Option A, and Option B+ further improved maternal outcomes with a reasonable cost-effectiveness ratio.

To develop an innovation based on this recommendation, stakeholders in Zimbabwe’s healthcare system can work together to ensure the widespread implementation of the WHO guidelines for PMTCT. This may involve training healthcare providers, improving access to CD4 testing and antenatal care, and ensuring the availability of ART medications. Additionally, efforts can be made to raise awareness among pregnant women about the importance of PMTCT and the benefits of following the recommended guidelines.

By implementing these innovations, access to maternal health services, particularly for HIV-infected pregnant women, can be improved, leading to better health outcomes for both mothers and infants.

AI Innovations Methodology

The study described in the provided text focuses on the cost-effectiveness of the World Health Organization (WHO) 2010 guidelines for prevention of mother-to-child HIV transmission (PMTCT) in Zimbabwe. The study used validated computer models to simulate the impact of different PMTCT regimens on maternal and infant outcomes, healthcare costs, and cost-effectiveness.

The methodology used in the study involved three linked computer models: the mother-to-child HIV transmission (MTCT) model, the Cost-effectiveness of Preventing AIDS Complications (CEPAC) adult model, and the CEPAC infant model. These models were used to simulate a cohort of pregnant, HIV-infected women in Zimbabwe and their infants. The models considered various PMTCT regimens, including no antenatal antiretroviral (ARV) drugs, single-dose nevirapine (sdNVP), WHO Option A, WHO Option B, and Option B+. The outcomes measured included maternal and infant life expectancy (LE) and lifetime healthcare costs.

To simulate the impact of the different PMTCT regimens, the models considered factors such as ANC costs, maternal HIV-related healthcare costs, infant healthcare costs, and medication costs. The models also took into account the risks of mother-to-child HIV transmission during pregnancy and breastfeeding, as well as the availability and effectiveness of CD4 testing and ARV medications. Sensitivity analyses were conducted to explore the impact of different assumptions and scenarios on the results.

The cost-effectiveness of the PMTCT regimens was evaluated using incremental cost-effectiveness ratios (ICERs), which represent the cost per year of life saved (YLS). The ICERs were compared to the 2008 Zimbabwe per capita gross domestic product and the range of ICERs for ART-related interventions in developing countries.

Overall, the study found that replacing sdNVP with Option A or Option B improved maternal and infant outcomes and saved money. Option B further increased health benefits and decreased costs compared to Option A. Option B+ had a similar ICER compared to Option B and further improved maternal outcomes.

In summary, the methodology used in the study involved the use of validated computer models to simulate the impact of different PMTCT regimens on maternal and infant outcomes and healthcare costs. The study provides valuable insights into the cost-effectiveness of the WHO 2010 guidelines for PMTCT in Zimbabwe.

Umbhali

Dima Health

Statistics:

Citations: 42

Identifiers:

DOI: 10.1093/cid/cis858

ISSN: 10584838

Research Areas:

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

Study Countries:

Botswana, Multi-Countries, South Africa, Zimbabwe

Study Design:

Cohort Study, randomised-control-trial

Study Approach:

Quantitative

Participants Gender:

Female

Yabelana ngalokhu: