Effects of undernutrition on survival of human immunodeficiency virus positive children on antiretroviral therapy

An institution-based retrospective cohort study was conducted for the period from the 1st of January, 2012 to the 28th of February, 2017 in Amhara Regional State Referral Hospitals (i.e., Debre Markos Referral Hospital, Felege Hiwot Comprehensive Specialized Hospital, and University of Gondar Comprehensive Specialized Hospital). These three hospitals serve more than 15 million people and care for the largest proportion of HIV clients in the Region. In addition to other services, all three referral hospitals provide chronic HIV care (ART) services. Currently, 1071 children receive ART follow up in these hospitals.

The source population were all HIV infected children (age < 15 years) whoa recorded initiation on ART in Amhara Regional State Referral Hospitals. The study population were all HIV-infected children who had ART follow up and recorded from the 1st of January, 2012 to the 28th of February, 2017 in any of the three selected hospitals, and whose chart was available during the data collection period. Study participants were taken proportionally from each of the three hospitals based on the total number of children in the ART unit of these hospitals. Children, who received ART for at least for one month between the 1st of January, 2012 to February 28, 2017, were included. However, children with incomplete baseline information were excluded from the study.

To calculate the required sample size, severe wasting, severe underweight, and severe stunting were considered as exposure variables. Moreover, severe underweight was considered as an independent variable since it yielded a maximum sample size. The sample size was determined by using a double population proportion formula, and calculated using Open Epi Version 3.To calculate our sample size, the following statistical assumptions were considered:P1:percent of exposed (severe underweight) with outcome (12.82%);P2:percent among the non-exposed with outcome (4%) estimated from a previous study conducted in Wolaita Health Facility, Southern Nations, Nationalities, and Peoples Region, Ethiopia [18]; Z α/2:reflects CI 95%;Z β: 80% power; and ratio of non-exposed to exposed 1:1. The final sample size was 177 for each group and the total sample size was 354. Finally, after adding 10% for contingency, the final sample size of our study was calculated as 390. The sample was proportionally allocated across each participating hospital, respecting medical records of children based on the previously stated criteria. From the isolated cards in each hospital, simple random sampling technique, computer-generating method was employed to select the study participants. The selected medical charts were followed for five years or until the termination of care.

The data abstraction tool was developed from a standardized ART entry and follow-up form currently used by the ART clinics. To ensure data quality, one-day training was given on the data abstraction tool and data collection process for both data collectors and supervisors. Necessary data were extracted by reviewing patients’ ART cards. The most recent laboratory test results prior to ART initiation were used as a baseline value. Both principal investigators and supervisors closely supervised the entire data collection process. All collected data were examined for completeness and consistency during the data management, storage, and analysis.

Data were entered into Epi-Data Version 3.1and analysis was done using STATA Version 13 statistical software. The WHO AnthroPlus Version 1.04 and ENA for Smart Software were used to generate the Z score (WAZ, HAZ and WHZ/BAZ) to define nutritional status. The assumption of Cox-proportional hazard regression model was checked using Schoenfeld residual test and variables having P-values> 0.1 were considered as fulfilling the assumption criteria. Finally, the outcome of each participant was dichotomized into censored or death. The Kaplan-Meier survival curve was used to estimate survival time after initiation of ART, and log rank tests were used to compare the survival curves. The Bivariate Cox-proportional hazards regression model was fitted for each explanatory variable. Moreover, those variables having p-value ≤0.25 in bivariable analysis were fit into the multivariable Cox-proportional hazards regression model. Hazard ratios with 95% confidence interval and p-values were used to measure the strength of association and to identify statistically significant predictors. In multivariable analysis, variables having P-values< 0.05 were considered as statistically significant predictors of mortality.

Undernutrition was defined as the child having either of H/Age Z-score < − 2, or W/Age Z-score < − 2 or W/H Z-score < − 2 SD [20, 21].

Moderate underweight was defined as children having W/Age Z-score < − 2 SD [20, 21].

Severe underweight was defined as children having W/Age Z-score < − 3 SD [20, 21].

Moderate stunting was defined as children having H/Age Z-score < − 2 SD [20, 21].

Severe stunting was defined as children having H/Age Z-score < − 3 SD [20, 21].

Moderate wasting was defined as children having W/H Z-score < − 2 SD [20, 21].

Severe wasting was defined as children having W/H Z-score < − 3 SD [20, 21].

Ethical clearance was obtained from an institutional review committee of the School of Nursing, College of Medicine and Health Sciences, University of Gondar. The ethics committee formally waived the need for formal written consent since the study was done through retrospective reviews of patient cards (charts). Permission letters were obtained from each hospital administration of the three participating entities. Since the study was a review of medical records, individual patients were minimally at risk for harm as confidentiality was likely to be achievable. To maintain ‘confidentiality, collected data were coded and locked in a separate room. After entry into the computer, all data were locked by password; as well, names and unique ART numbers were not included in the data collection forms.

Among the 390 records included in the final analysis about half (53.9%) were females, and the majority (85.4%) were from urban areas. The mean age of the cohort at the time of ART initiation was 6.9 years (SD ± 0.2 years). The mean age of the caregiver of the children was 32.9 years (SD ± 0.4 year) (Table 1).

Clinically more than half (58.8%) of the children started ART when classified as ‘mild’ according to the WHO HIV clinical disease stage (I&II). About three quarters (75.8%) of the children had achieved appropriate developmental milestones prior to ART initiation. Prior to ART initiation, 53.3% of the children had opportunistic infections. More than two thirds (70.0%) of the children had CD4 counts below the threshold for severe immunodeficiency. About 30.3% of the children had a history of regimen change throughout the entire follow up. From those who had a history of regimen change, toxicity or drug side effect (44.8%) was the most common reason followed by drug out of stock (24.6%) and clinical failure (9.8%). In addition, among those experiencing drug side effects (17.8%) during the follow-up period, anemia (30.8%) was the most common complaint followed by nausea (20.8%) and rash (12.3%) (Table 2).

At baseline, about one-fifth (20.3%) of the study participants were moderately underweight, 12.0% were moderately stunted, and 12.6% were moderately wasted. In addition, the proportions of presenting child malnutrition cases were classified as severe stunting (19.7%), severe wasting (13.9%), and severe underweight (15.1%) (Table 3).

Within a median follow-up period of 24.65 months with IQR (12- 39 months), 9.7% of the study participants died, 5.4% were lost to follow up, 14.4% were transferred out, leaving the remaining 70.5% alive. The overall mortality rate of the entire follow-up was 4.4 per 100 child years (95% CI: 3.2, 6.0). Regarding the time of death, 50%, 63%, and 68% of the deaths occurred within the first six, twelve, and eighteen months of ART initiation, respectively. The mean survival time of the entire follow-up was 56.4 months (95% CI: 53.7, 57.5). The cumulative probabilities of survival at 3, 6, 12, 24, and 60 months after initiation of ART were 0.966, 0.950, 0.935, 0.831, and 0.831, respectively. The cohort contributed a total of 10,376 child-months of follow-up.

To test the equality of survival curves for different categorical predictor variables the Cochran-Mantel Haenszel log rank test was used. The results showed that there was a significant difference in the survival function of different categorical variables; specifically, nutritional status (under or normal), hemoglobin (< 10 g/dl and ≥10 g/dl), CD4 count or percent (below and above the threshold), and WHO HIV clinical disease staging (i.e., mild to advanced).The mean survival time for children who were undernourished at the time of ART initiation was 50.6 months (SD±1.7), but 61.1 months (SD ± 0.6) for those who were well nourished. This difference was statistically significant with a P-value < 0.001 (Fig. 1).

In this study, children who had low hemoglobin levels (< 10 g/dl) had a lower survival time as compared to those with high hemoglobin level (≥10 g/dl). The mean survival time of children having low hemoglobin level was 39.6 months (SD±4.1) and the mean survival time of children having hemoglobin level ≥10 g/dl was 57.5 months (SD±0.9). This difference was statically significant with P-value < 0.001 (Fig. 2).

The mean survival time for children classified as WHOHIV clinical stages I or II at the time of ART initiation was 59.5 months (SD±0.9) as compared to those assessed as WHO HIV clinical stages III and IV with a mean survival time of 50.3 months (SD±1.9). This difference is statistically significant with P-value < 0.001 (Fig. 3).

The mean survival time for initiates withCD4 count or percent below the threshold was 53.9 months (SD ±1.3), which was lower than the mean survival time of individuals who had CD4 count or percent above the threshold with a mean survival time of 59.3 months (SD ±1. 2). This difference was statistically significant with P-value = 0.011 (Fig. 4).

In the bivariable analysis, being male, aged 5-15 years, living in rural areas, hemoglobin level < 10 g/dl, presence of OI, CD4 cell count or percentage below the threshold, categorized as WHO HIV clinical stages III&IV, underweight (moderate and severe), stunted (moderate and severe) and wasted (moderate and severe) were found to be significant predictors of mortality. In the multivariable Cox-regression analysis, only five variables were found to be predictors of mortality. The result of multivariable analysis revealed that children with advanced WHO HIV clinical stages (III and IV) were 2.6 times higher risk of death as compared to those with WHO HIV clinical stage (I and II) (AHR: 2.6, 95% CI: 1.1, 6.6). In this study, CD4 count was found to be another predictor of mortality. Children exhibiting CD4 cell count or percentages below the threshold were 5.2 times at higher risk of death as compared to cohort members below thresholds (AHR: 5.2, 95% CI: 1.9, 14.1). Moreover, initiates with hemoglobin levels less than 10 g/dl were at 3.2 times higher risk of death than those with hemoglobin levels greater than or equal to 10 g/dl (AHR: 3.2, 95% CI: 1.4, 7.4). Case presence of severe stunting at the beginning of ART showed 3.9 times higher risk of death than non-stunting cases (AHR: 3.9, 95% CI: 1.7, 9.4). Furthermore, children who were severely wasted were at 3.0 times higher risk of death as compared to those who were not wasted (AHR: 3.0, 95% CI: 1.3, 6.9) (Table 4).

This study experienced inconsistencies in ascertaining causes of death, especially for those who died at home. Loss to follow-up might also have included those died without being reported. Furthermore, important predictors of mortality, like viral load and micronutrient deficiency, were not considered. Despite the above limitations, the study was conducted over a significant period, which increases the period of observation, thereby increasing the number of events.