The association of malaria morbidity with linear growth, hemoglobin, iron status, and development in young Malawian children: A prospective cohort study

BMC Pediatrics, Volume 18, No. 1, Year 2018

Interprétation

Background: Although poor complementary feeding is associated with poor child growth, nutrition interventions only have modest impact on child growth, due to high burden of infections. We aimed to assess the association of malaria with linear growth, hemoglobin, iron status, and development in children aged 6-18 months in a setting of high malaria and undernutrition prevalence. Methods: Prospective cohort study, conducted in Mangochi district, Malawi. We enrolled six-months-old infants and collected weekly data for ‘presumed’ malaria, diarrhea, and acute respiratory infections (ARI) until age 18 months. Change in length-for-age z-scores (LAZ), stunting, hemoglobin, iron status, and development were assessed at age 18 months. We used ordinary least squares regression for continuous outcomes and modified Poisson regression for categorical outcomes. Results: Of the 2723 children enrolled, 2016 (74.0%) had complete measurements. The mean (standard deviation) incidences of ‘presumed’ malaria, diarrhea, and ARI, respectively were: 1.4 (2.0), 4.6 (10.1), and 8.3 (5.0) episodes/child year. Prevalence of stunting increased from 27.4 to 41.5% from 6 to 18 months. ‘Presumed’ malaria incidence was associated with higher risk of stunting (risk ratio [RR] = 1.04, 95% confidence interval [CI] = 1.01 to 1.07, p = 0.023), anemia (RR = 1.02, 95%CI = 1.00 to 1.04, p = 0.014) and better socio-emotional scores (B = – 0.21, 95%CI = – 0.39 to – 0.03, p = 0.041), but not with change in LAZ, haemoglobin, iron status or other developmental outcomes. Diarrhea incidence was associated with change in LAZ (B = – 0.02; 95% CI = – 0.03 to – 0.01; p = 0.009), stunting (RR = 1.02; 95% CI = 1.01 to 1.03; p = 0.005), and slower motor development. ARI incidence was not associated with any outcome except for poorer socio-emotional scores. Conclusion: In this population of young children living in a malaria-endemic setting, with active surveillance and treatment, ‘presumed’ malaria is not associated with change in LAZ, hemoglobin, or iron status, but could be associated with stunting and anemia. Diarrhea was more consistently associated with growth than was malaria or ARI. The findings may be different in contexts where active malaria surveillance and treatment is not provided. Trial registration: NCT00945698 (July 24, 2009) and NCT01239693 (November 11, 2010). The iLiNS-DOSE and iLiNS-DYAD-M studies were conducted in one public district hospital (Mangochi), one mission hospital (St Martins), and two rural public health centers (Lungwena and Namwera) in Mangochi District, Southern Malawi. The total catchment population of 180,000 largely subsisted on farming and fishing. In Malawian children aged < 5 years, the prevalence of reported fever (a proxy for malaria), diarrhea and ARI was 29, 22 and 5%, respectively, with seasonal fluctuations [17]. Malaria is endemic in Malawi and the study area has high malaria transmission with high temperature and frequent rainfall from October through April [18]. In the iLiNS-DOSE study, 6-mo old children were randomly allocated to one of five intervention groups provided with different doses or formulations of LNS or to a control group that did not receive LNS during the 12-mo study period, between November 2009 and May 2012. In the iLiNS-DYAD-M study, pregnant women < 20 weeks’ gestation were randomly allocated to one of three groups to receive iron and folic acid (IFA), multiple micronutrients (MMN) or a small-quantity (20 g) of LNS daily. After delivery, women in the IFA group received placebo tablets, while MMN and LNS supplementation was continued up to 6 mo postpartum. Children of mothers in the LNS group also received LNS 10 g twice daily from age 6 to 18 mo. This study was conducted from February 2011 to April 2015. Details of study design, randomization and enrolment for the two studies were explained in the main outcome papers [15, 16]. In both studies, research assistants visited the children’s homes every week from age 6 to 18 mo to interview the guardians about the child’s health in the previous 7 days using a structured questionnaire. The information was complemented by a picture calendar filled out by the guardians daily to aid memory of their children’s morbidity status. The use of maternal interviews as a means of collecting data on child morbidity has been validated in previous studies [19, 20]. The research assistants referred all cases of ‘presumed’ malaria (presence of fever) to the nearby health facility for treatment with lumefantrine/artemether, the nationally recommended antimalarial drug. The children were followed throughout the year, covering periods of both high and low malaria transmission. Anthropometric measurements were taken at age 6 mo and 18 mo. Study anthropometrists measured the infant’s length with a high-quality length board (Harpenden Infantometer; Holtain Limited) and recorded it to the nearest 1 mm. They weighed unclothed infants with electronic infant weighing scale (SECA 735; Seca GmbH & Co), recording to the nearest 10 g. The anthropometrists were trained and their measurement reliability was verified at the start of the study and at 6-mo intervals thereafter with methods adapted from the procedures used in the WHO Multicentre Growth Reference Study [21]. The anthropometrists calibrated all equipment with standard weights and length rods daily. We assessed iron status at age 6 mo and 18 mo by measuring the zinc protoporphyrin (ZPP) concentration in unwashed venous blood sample using a hematofluorometer (206D, AVIV Biomedical Inc., Lakewood, NJ, USA). About 5–7 ml of blood was collected by venepuncture using a 23-gauge needle into 7.5 ml evacuated, trace element-free polyethylene tubes containing lithium heparin (Sarstedt AG & Co, Nümbrecht, Germany). The samples were kept covered in aluminium and away from light, in a refrigerator or on ice, and processed within 2 h of collection. We measured blood hemoglobin (Hb) concentration at age 6 mo and 18 mo from a drop of blood taken from a finger prick and collected in a microcuvette. Hb analysis was conducted on-site using a Hemo-Cue instrument (Hemocue 201+, HemoCue® AB, Ängelholm, Sweden). We assessed fine and gross motor development at age 18 mo using the Kilifi Developmental Inventory (KDI) developed in Kenya [22]. Language development was assessed using a 100-word vocabulary checklist by maternal interview based on the MacArthur-Bates Communicative Development Inventory [23] adapted for the local languages, and 18-mo socio-emotional development was assessed using the Profile of Social and Emotional Development (PSED), also developed in Kenya. The child’s mood during the KDI assessment was rated as positive (smiling/laughing) or not positive (crying/inconsolable, changeable/mood swings, or no visible emotions). The child’s interaction with the assessor during the KDI was rated as positive (friendly) or not positive (avoidant and withdrawn, clings to family member, hesitant/when approached will accept reluctantly, difficult to engage in tasks, or inappropriate approaches to the assessor). The child’s activity level during the KDI was rated as positive (active and maintains interest) or not positive (unarousable, sleepy and can hardly be awakened, sleepy but easily awakened, does not spontaneously engage in activity, and awake but loses interest). The KDI, vocabulary, and PSED scores showed high inter-rater agreement and moderate to high test-retest reliability in this study setting [24, 25]. We used a presumptive diagnosis of malaria derived from episodes of fever during the previous week, reported by the guardians. To ensure the diagnoses were mutually exclusive, we created an algorithm whereby any fever with a diarrhea episode (three or more loose stools in 24 h) was categorized as diarrhea; any fever in the presence of any respiratory symptoms (cough, rapid or difficult breathing and nasal discharge) was categorized as ARI. ‘Presumed’ malaria was defined as any fever episode in the absence of diarrhea and respiratory symptoms. An episode of ‘presumed’ malaria, ARI or diarrhea was defined as the period starting from the day the child had the symptoms when preceded by at least 2 days of no symptoms or no data. The episode ended on the last day the child had the symptoms which was then followed by at least 2 symptom-free days. Incidence of ‘presumed’ malaria, ARI or diarrhea for each child from age 6 to 18 mo was calculated as total episodes / total follow up years at risk. Longitudinal prevalences of common childhood symptoms (fever, diarrhea, and cough) from age 6 to 18 mo were defined as the number of days with the symptom divided by the total number of days of observation for each child [26]. We calculated age- and sex-standardized anthropometric indices [length-for-age z score (LAZ), weight-for-age z score (WAZ), and weight-for-length z score (WLZ)] based on the WHO Child Growth Standards [21] and considered values below – 2.0 indicative of underweight, stunting and wasting, respectively. Change in LAZ for each child was calculated as the difference between LAZ at age 18 mo and LAZ at age 6 mo. Iron deficiency at age 6 mo and 18 mo was defined as whole blood ZPP > 70 μmol/mole heme [27]. Anemia at age 6 mo was defined as blood Hb concentration < 105 g/L [28] while anemia at age 18 mo was defined as blood Hb concentration < 110 g/L [29]. From the child development data at age 18 mo, fine motor scores were calculated as the sum of 34 KDI fine motor items, each scored 0 or 1, gross motor scores were calculated as the sum of 35 KDI gross motor items, each scored 0 or 1 [22] and vocabulary score was the maternal-reported child expressive vocabulary out of the 100-word checklist. For these outcomes, moderate to severe delay was defined as the bottom 25% of the sample. The socio-emotional score was calculated as the sum of 19 PSED items. Moderate to severe delay was defined as the top 25% of our sample (a higher score indicates less advanced socio-emotional development). We included in the analysis children who had outcomes measured at age 18 mo. For all continuous outcomes, we used ordinary least squares regression to assess the association between malaria incidence and each outcome; and for all binary outcomes, we used modified Poisson regression (with a robust variance estimator) [30]. We first assessed whether the relationship between the predictor and each outcome differed between the two studies. However, the interaction term was not statistically significant indicating that this relationship was not different between the two studies therefore we pooled data from the two cohorts. We then constructed multivariate models to determine which variables independently predicted the outcomes. We included all theoretically relevant variables, regardless of whether they were statistically significant or not after the bivariate analysis. The following variables collected at age 6 mo were included in the models: child sex, LAZ, WLZ, Hb, iron status, maternal education and household food insecurity access (HFIA) score generated by summing the value of responses to nine questions regarding food insecurity [31]. We also included in the models, from age 6 to 18 mo, the incidence of diarrhea and ARI, and whether the child received an intervention (LNS) or not. For the risk of stunting at age 18 mo, we included in the model stunting at age 6 mo (in place of LAZ). In addition, all developmental outcomes were adjusted for the child’s mood, activity level, age and interaction with the assessor. We assessed collinearity among the variables (e.g. LAZ vs WLZ at age 6 mo). If the variables were highly collinear (> 0.5), we dropped the one that was less strongly associated with the outcomes. We accounted for intracluster correlation due to twins using generalised estimating equations [32]. We also performed exploratory analyses by using frequency of malaria episodes (from age 6 to 18 mo) as a categorical variable (no episode, one episode, and > 1 episodes groups). In addition, we conducted stratified analyses by stunting at age 6 mo. Although we performed bivariate analyses for each individual variable, we will only report the results from multivariate analysis. We used Stata version 14 (StataCorp, Texas, USA) for all the analyses.

Résumé de l’IA

Study Justification:

This study aimed to assess the association of malaria with linear growth, hemoglobin, iron status, and development in children aged 6-18 months in a setting of high malaria and undernutrition prevalence. The study aimed to fill a gap in knowledge regarding the impact of malaria on child growth and development, particularly in areas with high malaria transmission and undernutrition.

Highlights:

– The study enrolled 2,723 children aged 6 months and collected weekly data on malaria, diarrhea, and acute respiratory infections until age 18 months.
– The prevalence of stunting increased from 27.4% to 41.5% from 6 to 18 months.
– ‘Presumed’ malaria incidence was associated with higher risk of stunting, anemia, and better socio-emotional scores.
– Diarrhea incidence was associated with slower linear growth, stunting, and slower motor development.
– Malaria was not associated with change in linear growth, hemoglobin, or iron status.
– The findings suggest that diarrhea has a more consistent impact on growth than malaria or acute respiratory infections.

Recommendations:

Based on the study findings, the following recommendations can be made:

1. Improve malaria prevention and treatment strategies, particularly in areas with high malaria transmission and undernutrition prevalence.
2. Enhance efforts to prevent and treat diarrhea in young children, as it has a significant impact on growth and development.
3. Implement interventions to address stunting and anemia, which are associated with ‘presumed’ malaria and diarrhea.

Key Role Players:

To address the recommendations, the following key role players are needed:

1. Health policymakers and government officials responsible for malaria control and child health programs.
2. Healthcare providers, including doctors, nurses, and community health workers, who can implement malaria prevention and treatment strategies and provide care for children with diarrhea.
3. Researchers and scientists who can further investigate the association between malaria and child growth and development and develop effective interventions.

Cost Items:

While the actual cost of implementing the recommendations will vary depending on the context, some key cost items to consider in planning the recommendations include:

1. Procurement and distribution of malaria prevention and treatment tools, such as insecticide-treated bed nets and antimalarial drugs.
2. Training and capacity building for healthcare providers on malaria prevention, diagnosis, and treatment.
3. Development and implementation of diarrhea prevention and management programs, including provision of oral rehydration solution and hygiene education.
4. Implementation of interventions to address stunting and anemia, such as nutritional supplementation and micronutrient fortification.
5. Monitoring and evaluation of the interventions to assess their impact and make necessary adjustments.
Please note that the cost items provided are general considerations and may not capture all the specific costs associated with implementing the recommendations.

Force de la preuve

The strength of evidence for this abstract is 7 out of 10.
The evidence in the abstract is rated 7 because it presents findings from a prospective cohort study with a large sample size. The study design allows for the assessment of associations between malaria and various outcomes in young Malawian children. However, the evidence could be strengthened by providing more details on the statistical methods used and addressing potential confounding factors. Additionally, the abstract could benefit from a clearer statement of the main findings and their implications.

Abstrait

The iLiNS-DOSE and iLiNS-DYAD-M studies were conducted in one public district hospital (Mangochi), one mission hospital (St Martins), and two rural public health centers (Lungwena and Namwera) in Mangochi District, Southern Malawi. The total catchment population of 180,000 largely subsisted on farming and fishing. In Malawian children aged < 5 years, the prevalence of reported fever (a proxy for malaria), diarrhea and ARI was 29, 22 and 5%, respectively, with seasonal fluctuations [17]. Malaria is endemic in Malawi and the study area has high malaria transmission with high temperature and frequent rainfall from October through April [18]. In the iLiNS-DOSE study, 6-mo old children were randomly allocated to one of five intervention groups provided with different doses or formulations of LNS or to a control group that did not receive LNS during the 12-mo study period, between November 2009 and May 2012. In the iLiNS-DYAD-M study, pregnant women 70 μmol/mole heme [27]. Anemia at age 6 mo was defined as blood Hb concentration < 105 g/L [28] while anemia at age 18 mo was defined as blood Hb concentration 0.5), we dropped the one that was less strongly associated with the outcomes. We accounted for intracluster correlation due to twins using generalised estimating equations [32]. We also performed exploratory analyses by using frequency of malaria episodes (from age 6 to 18 mo) as a categorical variable (no episode, one episode, and > 1 episodes groups). In addition, we conducted stratified analyses by stunting at age 6 mo. Although we performed bivariate analyses for each individual variable, we will only report the results from multivariate analysis. We used Stata version 14 (StataCorp, Texas, USA) for all the analyses.

Matériaux

N/A

Innovations

Based on the information provided, it is difficult to identify specific innovations for improving access to maternal health. The study mentioned focuses on the association of malaria morbidity with various health outcomes in young Malawian children, rather than directly addressing maternal health. To recommend innovations for improving access to maternal health, it would be helpful to have more information specifically related to maternal health challenges and potential solutions.

AI Innovations Description

Based on the provided description, it appears that the study aimed to assess the association of malaria with various health outcomes in children aged 6-18 months in a setting with high malaria and undernutrition prevalence. The study collected data on ‘presumed’ malaria, diarrhea, acute respiratory infections (ARI), linear growth, hemoglobin, iron status, and development in the children.

The study found that ‘presumed’ malaria incidence was associated with a higher risk of stunting, anemia, and better socio-emotional scores. Diarrhea incidence was associated with a decrease in linear growth, stunting, and slower motor development. ARI incidence was not significantly associated with any outcome except for poorer socio-emotional scores.

Based on these findings, a recommendation to improve access to maternal health and potentially reduce the impact of malaria on child health could be to implement interventions that focus on preventing and treating malaria in pregnant women and young children. This could include:

1. Providing pregnant women with malaria prevention measures such as insecticide-treated bed nets and intermittent preventive treatment.
2. Ensuring access to early diagnosis and prompt treatment of malaria in pregnant women and young children.
3. Promoting and supporting exclusive breastfeeding, as it has been shown to have a protective effect against malaria.
4. Implementing comprehensive antenatal care programs that include regular screening and treatment for malaria.
5. Strengthening health systems and improving access to quality healthcare services in malaria-endemic areas.
6. Conducting community education and awareness campaigns to increase knowledge about malaria prevention and treatment.

By implementing these recommendations, it is possible to improve access to maternal health and reduce the burden of malaria on maternal and child health outcomes.

AI Innovations Methodology

Based on the provided information, here are some potential recommendations for improving access to maternal health:

1. Strengthening Antenatal Care (ANC) Services: Enhance the quality and availability of ANC services by ensuring regular check-ups, providing comprehensive health education, and promoting early detection and management of maternal health issues.

2. Mobile Health (mHealth) Interventions: Utilize mobile technology to deliver maternal health information, reminders, and appointment notifications to pregnant women, especially in remote areas with limited access to healthcare facilities.

3. Community-Based Maternal Health Programs: Implement community-based programs that involve trained community health workers to provide essential maternal health services, including prenatal care, postnatal care, and family planning, within the community.

4. Improving Transportation and Infrastructure: Enhance transportation systems and infrastructure to ensure pregnant women can easily access healthcare facilities, especially in rural and remote areas.

5. Maternal Health Insurance: Establish or expand health insurance schemes that specifically cover maternal health services, ensuring that financial barriers do not prevent women from accessing necessary care.

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

1. Define the indicators: Identify key indicators that reflect access to maternal health, such as the number of antenatal care visits, percentage of deliveries attended by skilled birth attendants, and maternal mortality rate.

2. Collect baseline data: Gather data on the current status of the selected indicators in the target population or region.

3. Define the intervention scenarios: Develop different scenarios based on the recommendations, specifying the extent and coverage of each intervention.

4. Simulate the impact: Use mathematical modeling or simulation techniques to estimate the potential impact of each intervention scenario on the selected indicators. This may involve analyzing historical data, conducting surveys or interviews, and applying statistical models.

5. Compare and evaluate the scenarios: Compare the simulated outcomes of each intervention scenario to the baseline data and evaluate the potential improvements in access to maternal health. Consider factors such as cost-effectiveness, feasibility, and sustainability.

6. Refine and prioritize interventions: Based on the simulation results, refine the interventions and prioritize those with the highest potential impact on improving access to maternal health.

7. Implement and monitor: Implement the recommended interventions and closely monitor the progress and outcomes. Continuously evaluate and adjust the interventions based on real-time data and feedback.

It is important to note that the specific methodology for simulating the impact may vary depending on the available data, resources, and context. Consulting with experts in the field of maternal health and utilizing evidence-based approaches can further enhance the accuracy and reliability of the simulation.

Auteur

Dima Health

Statistics:

Citations: 6

Identifiers:

DOI: 10.1186/s12887-018-1378-2

Research Areas:

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

Study Countries:

Kenya, Malawi, Multi-Countries

Study Design:

Cohort Study, Cross Sectional Study, Exploratory Study, randomised-control-trial

Study Approach:

Quantitative

Participants Gender:

Female

Partagez ceci :