#PAGE_PARAMS# #ADS_HEAD_SCRIPTS# #MICRODATA#

Mortality and recovery following moderate and severe acute malnutrition in children aged 6–18 months in rural Jharkhand and Odisha, eastern India: A cohort study


Authors: Audrey Prost aff001;  Nirmala Nair aff002;  Andrew Copas aff001;  Hemanta Pradhan aff002;  Naomi Saville aff001;  Prasanta Tripathy aff002;  Rajkumar Gope aff002;  Shibanand Rath aff002;  Suchitra Rath aff002;  Jolene Skordis aff002;  Sanghita Bhattacharyya aff003;  Anthony Costello aff002;  Harshpal S. Sachdev aff004
Authors place of work: University College London, Institute for Global Health, London, United Kingdom aff001;  Ekjut, Chakradharpur, Jharkhand, India aff002;  Public Health Foundation of India, New Delhi, India aff003;  Sitaram Bhartia Institute of Science and Research, New Delhi, India aff004
Published in the journal: Mortality and recovery following moderate and severe acute malnutrition in children aged 6–18 months in rural Jharkhand and Odisha, eastern India: A cohort study. PLoS Med 16(10): e32767. doi:10.1371/journal.pmed.1002934
Category: Research Article
doi: https://doi.org/10.1371/journal.pmed.1002934

Summary

Background

Recent data suggest that case fatality from severe acute malnutrition (SAM) in India may be lower than the 10%–20% estimated by the World Health Organization (WHO). A contemporary quantification of mortality and recovery from acute malnutrition in Indian community settings is essential to inform policy regarding the benefits of scaling up prevention and treatment programmes.

Methods and findings

We conducted a cohort study using data collected during a recently completed cluster-randomised controlled trial in 120 geographical clusters with a total population of 121,531 in rural Jharkhand and Odisha, eastern India. Children born between October 1, 2013, and February 10, 2015, and alive at 6 months of age were followed up at 9, 12, and 18 months. We measured the children’s anthropometry and asked caregivers whether children had been referred to services for malnutrition in the past 3 months. We determined the incidence and prevalence of moderate acute malnutrition (MAM) and SAM, as well as mortality and recovery at each follow-up. We then used Cox-proportional models to estimate mortality hazard ratios (HRs) for MAM and SAM. In total, 2,869 children were eligible for follow-up at 6 months of age. We knew the vital status of 93% of children (2,669/2,869) at 18 months. There were 2,704 children-years of follow-up time. The incidence of MAM by weight-for-length z score (WLZ) and/or mid-upper arm circumference (MUAC) was 406 (1,098/2,704) per 1,000 children-years. The incidence of SAM by WLZ, MUAC, or oedema was 190 (513/2,704) per 1,000 children-years. There were 36 deaths: 12 among children with MAM and six among children with SAM. Case fatality rates were 1.1% (12/1,098) for MAM and 1.2% (6/513) for SAM. In total, 99% of all children with SAM at 6 months of age (227/230) were alive 3 months later, 40% (92/230) were still SAM, and 18% (41/230) had recovered (WLZ ≥ −2 standard deviation [SD]; MUAC ≥ 12.5; no oedema). The adjusted HRs using all anthropometric indicators were 1.43 (95% CI 0.53–3.87, p = 0.480) for MAM and 2.56 (95% CI 0.99–6.70, p = 0.052) for SAM. Both WLZ < −3 and MUAC ≥ 11.5 and < 12.5 were associated with increased mortality risk (HR: 3.33, 95% CI 1.23–8.99, p = 0.018 and HR: 3.87, 95% CI 1.63–9.18, p = 0.002, respectively). A key limitation of our analysis was missing WLZ or MUAC data at all time points for 2.5% of children, including for two of the 36 children who died.

Conclusions

In rural eastern India, the incidence of acute malnutrition among children older than 6 months was high, but case fatality following SAM was 1.2%, much lower than the 10%–20% estimated by WHO. Case fatality rates below 6% have now been recorded in three other Indian studies. Community treatment using ready-to-use therapeutic food may not avert a substantial number of SAM-related deaths in children aged over 6 months, as mortality in this group is lower than expected. Our findings strengthen the case for prioritising prevention through known health, nutrition, and multisectoral interventions in the first 1,000 days of life, while ensuring access to treatment when prevention fails.

Keywords:

Death rates – children – India – Infants – anthropometry – malnutrition

Introduction

In 2017, around 50 million children under 5 years globally were acutely malnourished [1]. Severe acute malnutrition (SAM) is defined as weight-for-height z score (WHZ)/weight-for-length z score (WLZ) < −3 standard deviation (SD) of the World Health Organization (WHO) 2006 Growth Standards, or mid-upper arm circumference (MUAC) < 11.5 cm [2]. Moderate acute malnutrition (MAM) is defined as WHZ/WLZ ≥ −2 and < −3 or MUAC ≥ 11.5 cm and < 12.5 cm [2]. Both MAM and SAM increase children’s risk of dying: a pooled analysis of 10 longitudinal studies from Asia, Africa, and South America found that children with moderate and severe wasting had 3- and 9-fold increased mortality rates, respectively, compared with children with WHZ > −1 [3]. Drawing on data collected mostly from hospitalised children before the advent of community-based management of acute malnutrition (CMAM), WHO estimated that between 10% and 20% of children with SAM generally die within 2–3 months without treatment, without discriminating between children with and without medical complications [46].

Nearly 18% of all children under 5 years globally live in India (121 out of 679 million), as do half of all children under 5 years affected by wasting (around 25.5 million out of 50.5 million) [1,7]. Indian policy makers, scholars, and activists relentlessly call for increased public funding to support the health, nutrition, sanitation, and social protection interventions that could reduce undernutrition [810]. Despite these efforts, scaling up preventive supplementary nutrition and detecting children with acute malnutrition has proved challenging. The Integrated Child Development Services’ (ICDS) Anganwadi (nutrition) workers should normally give supplementary food to pregnant and breastfeeding women, children under 3 years, and adolescent girls. They should also measure children’s WHZ monthly and refer severely wasted children to malnutrition treatment centres (MTCs) [10]. In 2014, however, a nationally representative survey found that only 21% of children aged 6–35 months received supplementary food at least 21 days per month [11]. When children with SAM were found and referred to MTC, families often feared the length and cost of hospital care [12]. There are currently no national-level data on the proportion of children with SAM who are identified and treated and few data on mortality following acute malnutrition in the community [9].

Using the Lives Saved Tool (LiST), the 2013 Lancet Commission on Maternal and Child Undernutrition estimated that scaling up outpatient feeding with ready-to-use therapeutic foods (RUTFs) for MAM and SAM at 90% coverage could save an estimated 435,210 children under 5 years every year [13,14]. Previous studies have suggested that mortality from acute malnutrition may be lower in India than in other settings [1517]. Measuring actual mortality rates from MAM and SAM for children in India is critical to understand how many deaths could be prevented by scaling up treatment.

In this analysis, we estimated the prevalence and incidence of MAM and SAM, referrals, mortality, and recovery in a cohort of children aged 6–18 months in Jharkhand and Odisha, two Indian states with high levels of undernutrition, in the context of ordinary detection and treatment protocols from the ICDS, and with no ongoing CMAM programme.

Methods

Design

We conducted a cohort study as a secondary data analysis nested within a cluster-randomised controlled trial conducted between 2013 and 2016. The original trial tested a community intervention to improve linear growth among children under 2 years in rural eastern India through a participatory learning and action cycle of meetings with women’s groups and monthly visits for all mothers from the third trimester of pregnancy until a child’s second birthday. The trial was registered as ISCRTN 51505201 and Clinical Trials Registry of India number 2014/06/004664 [18]. This cohort study is reported in accordance with the Strengthening the Reporting of Observational Studies in Epidemiology (STROBE) guideline (S1 STROBE Checklist).

Setting

The trial from which our cohort data are drawn took place in two districts: West Singhbhum, in Jharkhand, and Kendujhar, in Odisha. Both districts had high levels of child undernutrition: in 2015–2016, 38% of children under 5 years in West Singhbhum were wasted (13.5% severely wasted), as were 19% of children in Kendujhar (5% severely wasted) [7]. Over 75% of the population in the trial study areas belonged to Adivasi communities (Hindi: original inhabitants—i.e., indigenous), also known as Scheduled Tribes. Most families were engaged in agricultural labour, and 46% of women could read [18]. In total, 61% of households had electricity, and 1% had an improved toilet [18]. ICDS had unequal coverage in the study areas: we witnessed multiple interruptions in the provision of iron and folic acid, deworming tablets, and supplementary nutrition between 2013 and 2016. In the study clusters, village-based Anganwadi workers weighed children whose mothers attended monthly Village Health and Nutrition Days, offered supplementary nutrition to moderately underweight children, and referred those who were severely underweight to the MTC. Three treatment centres served the study communities: two in West Singhbhum and one in Kendujhar. They admitted children with WHZ < −3 SD or MUAC < 11.5 cm for inpatient treatment.

Participants

In the trial that provided data for this study, 120 clusters were purposively created to approximate Anganwadi worker catchment areas of 1,000 people each [19]. Community-based informants identified all women in the third trimester of pregnancy residing in these clusters and invited them to participate in the study. All women who agreed were visited again within 72 hours of the birth, as well as 3, 6, 9, 12, and 18 months after the birth. For this cohort study, eligible participants were all singleton children born to pregnant women recruited between October 1, 2013, and February 10, 2015 (the trial recruitment period), and who were alive at 6 months of age. Data collectors made a minimum of three attempts to find children at each follow-up. We excluded data from infants younger than 6 months for three reasons. First, these infants are not currently targeted by community-based detection, referral, and treatment programmes for acute malnutrition in India. Second, other studies on mortality and recovery following MAM and SAM in India included children older than 6 months, and we wanted our analyses to be comparable with these. Finally, we had substantial missing data for WLZ or MUAC within 72 hours of birth (39.6%, or 1,188/3,001) because many mothers and infants were still in hospital or away from their homes; these missing data made it challenging to explore the association between birth anthropometry and mortality.

Variables

We defined an episode of SAM as being newly identified with WLZ < −3, MUAC < 11.5 cm, and/or bilateral pitting oedema at 6, 9, or 12 months after not being SAM or missing at the previous follow-up. Similarly, we defined an episode of MAM as being newly identified with WLZ between −3 and −2 and/or MUAC between 11.5 and 12.5 cm at 6, 9, or 12 months after not being MAM or missing at the previous follow-up. Children could be acutely malnourished at two or more consecutive follow-ups; we reported such cases as a single episode of acute malnutrition. For example, a child found with SAM at both 6 and 9 months was counted as having a single episode of SAM. A child with SAM at 6 months who recovered at 9 months but was SAM again at 12 months was counted as having two episodes. Recovery was defined as WLZ ≥ 2 SD, MUAC ≥ 12.5, and no oedema. We considered a child to have died from acute malnutrition if they were acutely malnourished at the last follow-up before death (e.g., if a child was acutely malnourished at 6 months and died before the next follow-up at 9 months). If a child was SAM at 6 months, recovered at 9 months, and died at 10 months, the child was not considered to have died from SAM. The case fatality rate was calculated from among incident cases of MAM/SAM only.

Measurement

Data collectors received 5 days of training on anthropometry, followed by 7 days of field practice. They measured children’s length using Shorr boards with a precision of 0.1 cm, their weight using Tanita BD-590 scales with 10-g graduations, and MUAC using UNICEF tapes with a precision of 0.1 cm. Data collectors also took part in three technical error of measurement (TEM) exercises: two before and one during the trial. In the first TEM, reliability coefficient values (R) were consistently over 0.95 for weight but below 0.5 for length and MUAC, which led to retraining and two further TEM exercises for length and MUAC. In the second and third TEMs, the average R was 0.98 for length and 0.78 for MUAC [20]. The third TEM took place in November 2014—i.e., nearly halfway through data collection. At each follow-up, data collectors checked whether the child was alive and asked whether they had ever been referred to an Anganwadi worker or MTC since the last visit. In total, 11% of interviews and measurements were conducted with a supervisor present. We had information on whether the children were alive at the last visit before migration. Data collectors sought to find each mother at least three times at each follow-up. Data collectors referred all children with WLZ < −3, oedema, or MUAC < 11.5 cm to local Anganwadi workers. This method was chosen to ensure that we did not create a parallel system for referrals to onwards facility-based treatment in MTC or bypass supplementary nutrition programmes.

Statistical methods

We had no formal written analysis plan but took key decisions and drafted dummy tables prior to the analysis. All children recruited in the original trial were included in the analysis. We described the mothers’ and children’s socioeconomic characteristics and then examined differences between children retained in the cohort and those lost to follow-up using chi-squared tests for categorical variables and t tests for continuous variables. We used the zscore06 macro in Stata 14 to generate z scores of 2006 WHO Growth Standards and excluded WLZ values < −5 and > 5 as implausible, as recommended in WHO guidance [21]. We checked and flagged any cases in which height and weight did not increase over an interval of 3 months. We then calculated the prevalence and incidence of MAM and SAM at 6, 9, 12, and 18 months. Within each time period (6–9 months, 9–12 months, 12–18 months), we checked whether surviving children remained SAM, became MAM, or recovered from acute malnutrition at the next follow-up.

We used Cox-proportional models to estimate minimally and fully adjusted hazard ratios (HRs) with 95% CIs for mortality following MAM and SAM by WLZ, MUAC, and oedema (as relevant) combined and then for individual indicators [22]. The variables indicating MAM and SAM were time varying and updated at each follow-up time to reflect their impact on the risk of death only during an episode. In this analysis, we included the effect of prevalent MAM and SAM. We used multiple imputation by chained equations to account for missing measurements of WLZ or MUAC for children who had measurements from at least one follow-up. Thirty imputations sets were created, with missing values imputed conditional on values for the same variable at other times and also on whether the child subsequently died and the time of death or censoring. In all Cox-proportional models, we used robust standard errors to account for correlation within clusters (villages). We included data from both the intervention and control arms of the trial to maximise power and present HRs both adjusted and unadjusted for trial allocation. The intervention reduced infant mortality (adjusted odds ratio [aOR]: 0.63; 95% CI 0.39–1.00, p = 0.05) and underweight at 18 months (aOR: 0.81; 95% CI 0.66–0.99, p = 0.04) but did not reduce wasting (aOR: 0.88; 95% CI 0.71–1.08, p = 0.22) or increase mean MUAC at 18 months (adjusted difference: 0.05; 95% CI −0.08 to 0.186, p = 0.44). Adjusted analyses included variables for child sex, trial allocation arm, and district. A minimal data set and STATA DO file are included to enable readers to replicate our analyses (S1 Data and S1 DO File).

Ethical considerations

We sought women’s individual informed consent in writing or by thumbprint during the enrolment interview in pregnancy and verbally before all subsequent interviews. The trial was reviewed and approved by the research ethics committee of the Public Health Foundation of India (June 2013, TRC-IEC-163/13), an independent ethics committee linked to Ekjut (May 2013, reference IEC/EKJUT/01), and University College London’s Research Ethics Committee (June 2013, reference 1881/002). The independent ethics committee linked to Ekjut approved this secondary data analysis after the completion of the trial.

Results

Retention and participants’ characteristics

Fig 1 shows the retention of participants in the study. In total, 2,869 singleton infants were eligible at 6 months, of which 36 died between 6 and 18 months, and 56 migrated permanently. We found 93% (2,669/2,869) of all children eligible at 6 months.

Fig. 1. Flowchart describing the retention of children in the study.
Flowchart describing the retention of children in the study.
MUAC, mid-upper arm circumference; WLZ, weight-for-length z score.

Table 1 describes mothers’ and children’s characteristics by follow-up status. Around half of infants were born in Kendujhar District in Odisha, and the other half were born in West Singhbhum, Jharkhand. Over two-thirds were born in Adivasi families. In total, 50.5% of infants were female, and 49.5% were male. Mothers’ mean height was 1.50 m (SD: 0.07), and children’s mean birth weight was 2.57 kg (SD: 0.4). We compared the characteristics of children with known vital status at 18 months with those of children lost to follow-up at 18 months. Children lost to follow-up were more likely to be from Jharkhand (72% of children lost to follow-up versus 48% of children with known status), female (59% of children lost to follow-up versus 50% of children with known status), and from poorer households (median multidimensional poverty score: −0.90 interquartile range [IQR]: −1.69, 0.63 for children lost to follow-up versus −0.56, IQR: −1.64, 1.39 for children with known status at 18 months).

Tab. 1. Characteristics of participants.
Characteristics of participants.

Case fatality and mortality incidence following MAM and SAM

Children had 1,098 episodes of MAM beginning between 6 and 18 months and a MAM incidence rate of 406 per 1,000 children-years (1,098/2,704 children-years). In all, 12 children died during an incident MAM episode, five within 6 months of the start of the episode, and seven after 6 months. The case fatality from MAM was 0.4% (5/1,098) within 6 months and 1.1% (12/1,098) overall.

Children had 513 episodes of SAM beginning between 6 and 18 months and a SAM incidence rate of 190 per 1,000 children-years (513/2,704 children-years). In total, six children died during an incident SAM episode, four within 6 months of the start of the episode, and two after 6 months. The case fatality for SAM was 0.8% (4/513) within 6 months and 1.2% overall (6/513).

Table 2 shows the mortality incidence rates for MAM and SAM, as well as unadjusted and adjusted associations between MAM and SAM incidence and short-term (i.e., within the episode) mortality. A total of 68 children could not be included in analyses with multiple imputation: 10 had no WLZ measurement at any follow-up, 55 had no MUAC measurement at any follow-up, and three were immediately censored at the 6 months’ visit. S1 Table shows the number of missing values for each WLZ, MUAC, and oedema variable. The mortality incidence rate for MAM was 19.1 per 1,000 children-years. The mortality incidence rate for SAM was 20.1 per 1,000 children-years. The adjusted HR for MAM using all anthropometric indicators was 1.43 (95% CI 0.53–3.87, p = 0.480) and 2.56 (95% CI 0.99–6.70, p = 0.052) for SAM (overall p = 0.073). Lower MUAC, lower WLZ, and the presence of oedema were associated with increased risk of mortality (p = 0.003, p = 0.060, and p = 0.059, respectively).

Tab. 2. Associations between anthropometric indicators of MAM or SAM and short-terma mortality.
Associations between anthropometric indicators of MAM or SAM and short-term<em class="ref"><sup>a</sup></em> mortality.

Nutritional status among survivors

S2 Table describes the prevalence of MAM and SAM at the start of each follow-up period (i.e., at 6, 9, and 12 months), along with the vital and nutritional status of children at the next follow-up. In total, 99% of all children with SAM at 6 months (227/230) were alive after 3 months, 40% (92/230) were still SAM, and 18% (41/230) had ‘recovered’ (WLZ ≥ −2 SD; MUAC ≥ 12.5; no oedema). Only 5% (32/584) of children with SAM at 6, 9, or 12 months were ever referred to an MTC. The coverage of preventive nutrition services was also unequal: for example, 66% (1,917/2,869) of children aged 6 months were weighed by an Anganwadi worker, but only 13% (382/2,869) had mothers who received nutrition counselling.

Outcomes up to 12 months after MAM and SAM

Fig 2 shows outcomes at 9, 12, and 18 months for children who were not undernourished or had MAM or SAM at 6 months. These were derived after multiple imputation for missing WLZ, MUAC, and oedema data. The proportions of children with MAM or SAM at 6 months who had died by 18 months were 1.3% and 1.1%, respectively. These were not very different, in absolute terms, to the proportion of non-acutely malnourished children who died (0.8%). Recovery from MAM and SAM was relatively low and stable over time. Recovery out of acute undernutrition was similar for MAM or SAM, particularly by 18 months.

Fig. 2. Long-term outcomes for children with and without acute malnutrition at 6 months, using a data set with multiple imputation.
Long-term outcomes for children with and without acute malnutrition at 6 months, using a data set with multiple imputation.
MAM, moderate acute malnutrition; SAM, severe acute malnutrition.

Discussion

We found a high incidence of MAM and SAM among rural, largely tribal communities of Jharkhand and Odisha. A substantial proportion (>40%) of children with MAM and SAM remained acutely malnourished for over 3 months, and 99% of children with SAM at 6 months survived for 3 months or more, suggesting that, in this context, MAM and SAM are persistent. WLZ < −3 was associated with increased mortality risk, as expected, but MUAC ≥ 11.5 and < 12.5 was associated with a greater mortality risk than MUAC < 11.5. The finding that children with MUAC ≥ 11.5 and < 12.5 had a higher mortality risk is counterintuitive and deserves further investigation. Anganwadi workers referred only 5% of SAM cases to MTC, highlighting a considerable treatment gap.

Our most salient finding is that SAM carried a much lower case fatality rate (1.2%) than expected from older, largely African studies and WHO estimates (10%–20%). If the two deceased children for whom we did not have any anthropometry data had died following SAM, the case fatality rate would have been 1.5% (8/513), still much below 10%–20%.

Three other Indian studies with different designs but broadly similar inclusion criteria offer data for comparison. The first was a follow-up study of children initially screened as having an MUAC < 11.5 cm as part of a multicentric trial in poor urban and rural communities in New Delhi, Udaipur, and Vellore [23]. Case fatality among children aged 6–23 months with MUAC < 11.5 cm was 4.3% (6/140) after 12 months [24]. A second study conducted in rural Uttar Pradesh found a case fatality of 2.7% among 409 children aged 6 months to 5 years followed up between 0.6 and 17.8 months after severe wasting [25]. In a third study from Bihar, Burza and colleagues followed up defaulters from a WHO-standard RUTF programme who had MUAC < 11.5 cm [26]. Case fatality among these defaulters—who tended to be younger children and girls—was 5.2% within 18 months (36/692). All of these case fatality rates, with varying durations of follow-up, are below WHO estimates (10%–20%) and closer to the 4% (range: 2%–7%) case fatality rate that a 2013 expert panel considered normal in the context of a CMAM programme [27].

There are at least four possible explanations for the considerable difference between case fatality rates in these recent Indian studies and the 10%–20% estimates drawn from older, largely African studies. First, the studies upon which WHO estimates are based included mostly hospitalised children who were more likely to have SAM with medical complications and, therefore, higher mortality rates [6].

A second possible explanation is that the most vulnerable children in our rural study areas died before reaching 6 months. In the trial’s control clusters, the infant mortality rate was 64 per 1,000 live births; 64% (116/181) of all infant deaths across both trial areas occurred in the first month of life, and 86% (157/181) occurred in the first 6 months [18]. In 2015, the prevalence of low birth weight per 100 births was greater in southern Asia than in sub-Saharan Africa (26.4%; uncertainty range [UR]: 18.6–35.2 versus 14.0%, UR: 12.2–17.2) [28]. Around half of neonatal deaths in India (370,000 of 698,000 neonatal deaths in 2015) are caused by prematurity or low birth weight, and these factors also accounted for 46.1% of all under-5 deaths in 2017 (95% uncertainty interval: 44.5–47.6) [29,30]. In rural India, undersize is probably taking its heaviest toll in the first 6 months of life, before treatment with RUTF becomes relevant.

A third source of variation in case fatality rates may lie in differences in infection burdens between South Asian and African settings. In 2017, the disability-adjusted life years rate for communicable maternal, neonatal, child, and nutritional diseases was 26,492 per 100,000 in sub-Saharan Africa, roughly double that in South Asia (13,197 per 100,000) [31]. HIV prevalence is 4.1% among 15–49-year-olds in sub-Saharan Africa versus 0.2% in South Asia, including India, and several studies have demonstrated that HIV infection interacts with undernutrition to increase the risk of death [3133].

A final explanation may lie in the developmental origins of adult health and disease. Mothers in our study areas had an average height of 1.5 m [17]. During pregnancy, half of them had an MUAC < 23 cm, and one-third of them did not have diets with minimum diversity [17]. Around one-third (33%) of infants were low birth weight, and over 65% were stunted by 18 months [18]. These data reflect intergenerational, chronic undernutrition inflicted by poverty [34]. Indian infants often have a ‘thin-fat’ phenotype: they have small abdominal viscera and low muscle mass but preserve body fat in utero that can track into birth and young adulthood, depending on the nutritional environment [35]. Studies have found that body fat–related measurements such as skinfold thickness, abdominal circumference, and MUAC are often similar between Indian babies and Western infants, despite low birth weight [36].The hidden adiposity of Indian infants may give small infants a survival advantage by acting as a form of energy reserve available to maintain body temperature and brain development in times of nutritional deprivation, albeit with adverse consequences for noncommunicable disease risk in later life [37]. It is therefore possible that thinness in infancy and early childhood does not carry the same mortality risk in this setting as in others. The interplay between undernutrition, immune dysfunction, and mortality risk is complex, as summarised in recent reviews [3840]. Integrating longitudinal immune assessments into ongoing trials of nutrition and water sanitation and hygiene (WASH) interventions will help elucidate when and how immune dysfunction and undernutrition interact and help better target public health interventions to lower mortality risk.

Our study had several strengths. To our knowledge, it is the largest Indian community-based longitudinal study of mortality following MAM and SAM in the absence of management of uncomplicated SAM with RUTF for children older than 6 months. The three TEM exercises undertaken by the data collection team enhance our trust in the accuracy of anthropometry data. We had information about vital status for 93% of infants eligible for follow-up at 6 months by the end of the study period.

Our study had three main limitations. We had missing anthropometry data for some children, including fully missing data for two of the 36 children who died. We attempted to address possible bias caused by missing data by using multiple imputation to provide more accurate estimates of mortality risk but were not able to use imputation for 68 children who had no WHZ or MUAC measurements at any time point. A second limitation is that we did not follow children up until 59 months of age. The study from Uttar Pradesh by Kapil and colleagues found a case fatality rate of 2.7% among children aged 6–60 months; this is higher than among the younger children in our study but still not within WHO’s estimated range [25]. Our results are therefore likely to be generalisable to young children aged 6–24 months in other rural, underserved Indian settings and may provide a modest underestimate of case fatality for children aged 6–59 months. Finally, monitoring and referral systems for SAM in the original trial differed from those available in the general population, and this may have contributed to lowering mortality. We have little evidence to support this hypothesis, however: infant mortality in the trial’s control area (63 per 1,000 live births) was similar to that reported in the 2011–2012 Annual Health Surveys for our two study districts (56 per 1,000 live births in Kendujhar and 58 in West Singhbhum), suggesting that the trial monitoring systems did not lead to large reductions in mortality in and of themselves [41].

If data from poor urban and rural communities in Delhi, Bihar, Uttar Pradesh and our own data from Jharkhand and Odisha are representative of the contemporary Indian situation, then case fatality rates following SAM in Indian children older than 6 months are substantially lower than those estimated from earlier studies conducted in African countries. In other Indian studies assessing progress following inpatient and/or community care for SAM, rates of recovery were often lower than recommended in SPHERE guidance, and relapse was common [4244]. For example, in a recent follow-up study of 150 children discharged from MTCs in Jharkhand, 52% of children had relapsed into severe wasting 2 months after discharge [45]. In light of these findings, scaling up outpatient RUTF treatment for children over 6 months without concurrently strengthening ICDS, WASH, and the social protection interventions that support the intergenerational prevention of undernutrition may not have the large effects on mortality predicted by the 2013 Lancet Maternal and Child Nutrition Series in India and other South Asian contexts [17]. Prevention can work: a recent intervention combining crèches, participatory meetings with women’s groups, and home visits reduced wasting, underweight, and stunting among children under 3 years old in Jharkhand and Odisha [46]. A recent UNICEF-led consultation aptly called for a new approach to wasting in South Asia, one that positions prevention as the ‘first priority’ and ensures access to treatment when prevention fails [47]. Our findings support such a strategy.

In conclusion, we found a high incidence of acute malnutrition among children older than 6 months in rural eastern India but a lower than expected case fatality rate following SAM. This finding has been replicated in at least three other Indian studies. Given that the risk of mortality is lower than expected among children older than 6 months and that many deaths occur because of prematurity or low birth weight during the neonatal period, outpatient treatment for SAM using RUTF for children over 6 months may be too late to avert a substantial number of deaths from undernutrition in Indian children. This further strengthens the case for prioritising prevention through known health, nutrition, and multisectoral interventions in the first 1,000 days of life.

Supporting information

S1 STROBE Checklist [docx]
STROBE, Strengthening the Reporting of Observational Studies in Epidemiology.

S1 Data [csv]

S1 DO File [do]

S1 Table [docx]

S2 Table [docx]


Zdroje

1. UNICEF, WHO, World Bank. Joint Child Malnutrition Estimates 2018. New York: UNICEF; 2019 [cited 2019 Jul 15]. Available from: https://data.unicef.org/resources/dataset/malnutrition-data/.

2. Black RE, Victora CG, Walker SP, Bhutta ZA, Christian P, de Onis M, et al. Maternal and child undernutrition and overweight in low and middle-income countries. Lancet. 2013; 382: 427–451. doi: 10.1016/S0140-6736(13)60937-X 23746772

3. Olofin I, McDonald CM, Ezzati M, Flaxman S, Black RE, Fawzi WW, et al. Associations of suboptimal growth with all-cause and cause-specific mortality in children under five years: a pooled analysis of ten prospective studies. PLoS ONE. 2013; 8(5): e64636. doi: 10.1371/journal.pone.0064636 23734210

4. World Health Organization. Community-based management of severe acute malnutrition: a joint statement by the World Health Organization, the World Food Programme, the United Nations System Standing Committee on Nutrition and the United Nations Children's Fund. Geneva: World Health Organization; 2007.

5. World Health Organization. Guideline: Updates on the management of severe acute malnutrition in infants and children. Geneva: World Health Organization; 2013.

6. Schofield C, Ashworth A. Why have mortality rates for severe malnutrition remained so high? Bull World Health Organ. 1996; 74: 223–229. 8706239

7. Ministry of Health and Family Welfare, Government of India. National Family Health Survey (NFHS-4), 2015–2016. Mumbai, India: International Institute of Population Sciences; 2017.

8. Menon P, McDonald CM, Chakrabarti S. Estimating the costs of delivering direct nutrition interventions at scale: national and subnational insights from India. Maternal and Child Nutrition. 2016; 12: 169–185. doi: 10.1111/mcn.12257 27187914

9. Rao S, Kaul V. India’s integrated child development services scheme: challenges for scaling up. Child: care, health and development. 2018; 34: 31–40.

10. Ministry of Women and Child Development. National Nutrition Mission: Administrative Guidelines. New Delhi, India: Government of India; 2018 Feb.

11. Ministry of Women and Child Development. Rapid Survey on Children: 2013–2014. New Delhi, India: Government of India; 2014.

12. Burtscher D, Burza S. Health-seeking behaviour and community perceptions of childhood undernutrition and community management of acute malnutrition (CMAM) programme in rural Bihar, India: a qualitative study. Public Health Nutrition. 2015; 18: 3234–3243. doi: 10.1017/S1368980015000440 25753193

13. Bhutta ZA, Das JK, Rizvi A, Gaffey MF, Walker N, Horton S, et al. Evidence-based interventions for improvement of maternal and child nutrition: what can be done and at what cost? Lancet. 2013; 382: 452–477. doi: 10.1016/S0140-6736(13)60996-4 23746776

14. Clermont A, Walker N. Nutrition Interventions in the Lives Saved Tool (LiST). The Journal of Nutrition. 2017; 11: 2132S–2140S.

15. Kapil U, Sareen N. Management of children with severe acute malnutrition. Indian Pediatrics. 2014; 51: 587–8.

16. Pelletier DL. The relationship between child anthropometry and mortality in developing countries: implications for policy, programs and future research. J Nutr. 1994; 124: 2047S–81S. doi: 10.1093/jn/124.suppl_10.2047S 7931716

17. Sachdev HS, Sinha S, Sareen N, Pandey RM, Kapil U. Survival and Recovery in Severely Wasted Under-five Children Without Community Management of Acute Malnutrition Programme. Indian Pediatrics. 2017; 10: 817–824.

18. Nair N, Tripathy P, Sachdev HS, Pradhan P, Bhattacharyya S, Gope R, et al. Effect of participatory women’s groups and counselling through home visits on children’s linear growth in rural eastern India (CARING trial): a cluster-randomised controlled trial. Lancet Global Health. 2017; 5: e1004–e1016. doi: 10.1016/S2214-109X(17)30339-X 28911749

19. Nair N, Tripathy P, Sachdev HS, Bhattacharyya S, Gope R, Gagrai S, et al. Participatory women’s groups and counselling through home visits to improve child growth in rural eastern India: protocol for a cluster randomised controlled trial. BMC Public Health. 2015; 15: 384. doi: 10.1186/s12889-015-1655-z 25886587

20. Ulijaszek SJ, Kerr DA. Anthropometric measurement error and the assessment of nutritional status. British Journal of Nutrition. 1999; 82: 165–177. doi: 10.1017/s0007114599001348 10655963

21. WHO Multicentre Growth Reference Study Group. WHO Child Growth Standards: Length/height-for-age, weight-for-age, weight-for-length, weight-for-height and body mass index-for-age: Methods and development. Geneva: World Health Organization; 2006.

22. Alkire S, Foster JE, Seth S, Santos ME, Roche JM, Ballon P. Multidimensional Poverty Measurement and Analysis. Oxford: Oxford University Press; 2015.

23. Bhandari N, Mohan SB, Bose A, Iyengar SD, Taneja S, Mazumder S, et al. Efficacy of three feeding regimens for home-based management of children with uncomplicated severe acute malnutrition: a randomised trial in India. BMJ Global Health. 2016; 1: e000144. doi: 10.1136/bmjgh-2016-000144 28588982

24. Taneja S, Rongsen-Chandola T, Mohan SB, Mazumder S, Bhandari N, Kaur J, et al. Mid upper arm circumference as a predictor of risk of mortality in children in a low resource setting in India. PLoS ONE. 2018; 13(6): e0197832. doi: 10.1371/journal.pone.0197832 29856757

25. Kapil U, Pandey RM, Bansal R, Pant B, Varshney AM, Yadav CP, et al. Mid-upper arm circumference in detection of weight-for-height z score below -3 in children aged 6–59 months. Public Health Nutr. 2018. doi: 10.1017/S1368980017004165

26. Burza S, Mahajan R, Marino E, Sunyoto T, Shandilya C, Tabrez M, et al. Seasonal effect and long-term nutritional status following exit from a Community-Based Management of Severe Acute Malnutrition program in Bihar, India. Eur J Clin Nutr. 2016; 70: 437–44. doi: 10.1038/ejcn.2015.140 26330147

27. Lenters LM, Wazny K, Webb P, Ahmed T, Bhutta ZA. Treatment of severe and moderate acute malnutrition in low- and middle-income settings: a systematic review, meta-analysis and Delphi process. BMC Public Health. 2013;13: S23. doi: 10.1186/1471-2458-13-S3-S23 24564235

28. Blencowe H, Krasevec J, de Onis M, Black RE, An X, Stevens GA, Borghi E, et al. National, regional, and worldwide estimates of low birthweight in 2015, with trends from 2000: a systematic analysis. Lancet Glob Health. 2019; 7: e849–60.

29. Million Deaths Study Collaborators. Changes in cause-specific neonatal and 1-59-month child mortality in India from 2000 to 2015: a nationally representative survey. Lancet. 2017; 390: 1972–1980. doi: 10.1016/S0140-6736(17)32162-1 28939096

30. India State-Level Disease Burden Initiative Malnutrition Collaborators. The burden of child and maternal malnutrition and trends in its indicators in the states of India: the Global Burden of Disease Study 1990–2017. Lancet Child Adolesc Health. 2019; doi: 10.1016/S2352-4642(19)30273-1

31. Global Burden of Disease Collaborative Network. Global Burden of Disease Study 2017 (GBD 2017) Results. Seattle: Institute for Health Metrics and Evaluation (IHME); 2018.

32. Fergusson P, Tomkins A. HIV prevalence and mortality among children undergoing treatment for severe acute malnutrition in sub-Saharan Africa: a systematic review and meta-analysis. Transactions of the Royal Society of Tropical Medicine and Hygiene. 2009; 103: 541–548. doi: 10.1016/j.trstmh.2008.10.029 19058824

33. Kerac M, Bunn J, Chagaluka G, Bahwere P, Tomkins A, Collins S, et al. Follow-Up of Post-Discharge Growth and Mortality after Treatment for Severe Acute Malnutrition (FuSAM Study): A Prospective Cohort Study. PLoS ONE. 2014; 9(6): e96030. doi: 10.1371/journal.pone.0096030 24892281

34. Shah A, Lerche J, Axelby R, Benbabaali D, Donegan B, Raj J, et al. Ground down by growth: tribe, caste, class and inequality in 21st Century India. London: Pluto Press; 2017.

35. Yajnik CS, Fall CHD, Coyaji KJ, Hirve SS, Rao S, Barker DJ, et al. Neonatal anthropometry: the thin-fat Indian baby. The Pune Maternal Nutrition Study. International Journal of Obesity. 2003; 27: 173–180. doi: 10.1038/sj.ijo.802219 12586996

36. Krishnaveni GV, Hill JC, Veena SR, Leary SD, Saperia J, Chachyamma KJ, et al. Truncal Adiposity is Present at Birth and in Early Childhood in South Indian Children. Indian Pediatrics. 2005; 42: 527–538. 15995269

37. Muthayya S, Dwarkanath P, Thomas T, Vaz M, Mhaskar A, Mhaskar R, et al. Anthropometry and body composition of south Indian babies at birth. Public Health Nutrition. 2006; 9: 896–903. 17010256

38. Bartz A, Mody A, Hornik C, Bain J, Muehlbauer M, Kiyimba T, et al. Severe Acute Malnutrition in Childhood: Hormonal and Metabolic Status at Presentation, Response to Treatment, and Predictors of Mortality. J Clin Endocrinol Metab. 2014; 99: 2128–2137. doi: 10.1210/jc.2013-4018 24606092

39. Maurya R, Bhattacharya P, Dey R, Nakhasi HL. Leptin Functions in Infectious Diseases. Front. Immunol. 2018; 9:2741. doi: 10.3389/fimmu.2018.02741 30534129

40. Bourke CD, Berkley JA, Prendergast AJ. Immune dysfunction as a cause and consequence of malnutrition. Trends Immunol. 2016; 37: 386–398. doi: 10.1016/j.it.2016.04.003 27237815

41. Ministry of Home Affairs, Office of the Registrar General and Census Commissioner. Annual Health Survey (2011–2). New Delhi, India: Government of India; 2013.

42. Garg A, Badgaiyan N, Singh K. Integrated program achieves good survival but moderate recovery rates among children with severe acute malnutrition in India. Am J Clin Nutr. 2013; 98:1335–42. doi: 10.3945/ajcn.112.054080 24067666

43. Singh K, Badgaiyan N, Ranjan A, Dixit HO, Kaushik A, Kushwala KP, et al. Management of children with severe acute malnutrition: experience of Nutrition Rehabilitation Centers in Uttar Pradesh, India. Indian Pediatrics. 2014; 51:21–5. doi: 10.1007/s13312-014-0328-9 24277964

44. Aguayo VM, Jacob S, Badgaiyan N, Chandra P, Kumar A, Singh K. Providing care for children with severe acute malnutrition in India: new evidence from Jharkhand. Public Health Nutrition. 2012; 17: 206–211. doi: 10.1017/S1368980012004788 23137752

45. Chaturvedi A, Patwari AK, Soni D. Progress of children with severe acute malnutrition in the malnutrition treatment centre rehabilitation program: evidence from a prospective study in Jharkhand, India. Nutrition Journal. 2018; 17: 69. doi: 10.1186/s12937-018-0378-2 30021572

46. Gope R, Tripathy P, Prasad V, Pradhan H, Sinha RK, Panda R, et al. Effects of participatory learning and action with women’s groups, counselling through home visits and crèches on undernutrition among children under three years in eastern India: a quasi-experimental study. BMC Public Health. 2019; 19: 962. doi: 10.1186/s12889-019-7274-3 31319828

47. UNICEF. Wasting in South Asia: Consultation on building the evidence base for the policy and programme response. New York: UNICEF; 2018 Nov 16.

Štítky
Interní lékařství

Článek vyšel v časopise

PLOS Medicine


2019 Číslo 10
Nejčtenější tento týden
Nejčtenější v tomto čísle
Kurzy

Zvyšte si kvalifikaci online z pohodlí domova

Aktuální možnosti diagnostiky a léčby litiáz
nový kurz
Autoři: MUDr. Tomáš Ürge, PhD.

Střevní příprava před kolonoskopií
Autoři: MUDr. Klára Kmochová, Ph.D.

Závislosti moderní doby – digitální závislosti a hypnotika
Autoři: MUDr. Vladimír Kmoch

Aktuální možnosti diagnostiky a léčby AML a MDS nízkého rizika
Autoři: MUDr. Natália Podstavková

Jak diagnostikovat a efektivně léčit CHOPN v roce 2024
Autoři: doc. MUDr. Vladimír Koblížek, Ph.D.

Všechny kurzy
Přihlášení
Zapomenuté heslo

Zadejte e-mailovou adresu, se kterou jste vytvářel(a) účet, budou Vám na ni zaslány informace k nastavení nového hesla.

Přihlášení

Nemáte účet?  Registrujte se

#ADS_BOTTOM_SCRIPTS#