Comparison of developmental milestone attainment in early treated HIV-infected infants versus HIV-unexposed infants: a prospective cohort study

HIV-infected infants participated in a randomized clinical trial (Optimizing Pediatric HIV-1 Therapy 03 (OPH03) with a 2-year pre-randomization period, in which infants attended monthly study visits, with data collection, prior to randomization (NCT00428116) [20]. As described previously, infants were identified at either maternal child health clinics or hospital wards in Nairobi. Enrollment eligibility criteria were HIV DNA PCR positive with confirmation, age <5 months, and no previous receipt of antiretroviral therapy, with the exception of prophylaxis for prevention of mother to child transmission (PMTCT). Following enrollment and adherence counseling, ART was initiated, generally within 2 weeks. Infants with no prior exposure to nevirapine (NVP) for PMTCT received a first-line regimen consisting of NVP plus 2 nucleoside reverse transcriptase inhibitors (generally zidovudine and lamivudine), and infants with prior NVP exposure received a first-line regimen consisting of this backbone, plus ritonavir-boosted lopinavir (LPV/r). Nearly all infants had received trimethoprim-sulfamethoxazole (cotrimoxazole) prophylaxis prior to or at enrollment. HIV-infected infants were enrolled from 2007 to 2009.

From 2011 to 2013, HIV-unexposed uninfected (HUU) infants were identified following routine HIV-testing offered to pregnant mothers at the Mathare North MCH Clinic in Nairobi. HIV seronegative mothers were recruited for infant participation in a 2-year cohort study involving similar study visit schedules as in the OPH03 study. Enrollment eligibility criteria were 1) age 0–4.5 months, 2) biological mother and infant with HIV-negative status, and 3) mother planned to reside within Nairobi for at least 2 years. Mother and infant HIV status were verified using an HIV rapid antibody test at enrollment. Maternal HIV-negative status was confirmed at 12 and 24 months during follow-up.

Following standardized questionnaires on sociodemographic and medical history, infants received a physical examination at enrollment and a blood sample was collected for CD4 testing and for HIV-infected infants, virologic testing. During follow-up, infants attended monthly visits at which a physical exam was administered with blood collection at 1-month and 3-monthly thereafter for HIV-positive infants, and 6-monthly for HUU infants.

Developmental milestones were assessed at enrollment and at monthly visits for the duration of follow-up. Milestones were adapted from the Denver Developmental Screening Test [21]. The same team of clinical officers performed study visits and assessed milestones. Caregivers self-reported the age at which the milestone had been achieved at monthly visits. Analyses presented here utilized the self-reported age wherever possible, and an estimated age (using the date of study visit at which the milestone was first noted by the clinician) was used in cases in which the self-reported age was missing. Sensitivity analyses including only the clinician-reported age gave similar results. Milestones included full neck control (defined as whether the infants could support his or her own head) (neck control), sitting with support (defined as whether the child could sit with a straight back on the caregiver’s lap or on the floor between the caregiver’s legs), sitting unsupported (defined as whether the child could sit on a flat surface or on the caregiver’s lap without needing support), walking with support (defined as whether the child could walk well with the help of someone holding one or both hands or when supporting self using furniture or a wall), walking unsupported (defined as whether the child could take a few steps without needing support), monosyllabic speech (defined as whether the infant was able to say one-syllable words or sounds, referring to a specific person or object) (speech), throwing toys (defined as whether the child could throw a toy such as a ball while playing), naming objects (defined as whether the caregiver reported that the child could point to and name common household items such as cups or plates). This analysis was focused primarily on milestones expected to occur within a few months of the 6-month on-ART visit, namely walking unsupported and speech.

In Nairobi, flow cytometry was performed to obtain enrollment and 6-monthly CD4 counts and percentages. Whole blood specimens were centrifuged using a Ficoll density gradient to separate plasma, which was cryopreserved at −70 ° C. Plasma HIV RNA levels were ascertained using the Gen-Probe HIV Viral Load Assay (San Diego, CA) in Seattle, WA [22]. Blood hemoglobin levels were assessed in Nairobi.

This study was a secondary analysis using data collected for infants participating in a randomized clinical trial (all infants with available milestone data were included) and a comparison group of infants enrolled (N = 100) during a later timeframe. Z-scores for weight-for-age (WAZ), height-for-age (HAZ), weight-for-height (WHZ) and head circumference-for-age (HCZ) were calculated using the 2006 WHO reference population [23]. Baseline characteristics were compared between HUU and HIV-infected infants using t-tests for continuous variables and chi-squared tests or Fisher’s exact tests, as appropriate, for dichotomous variables. Baseline cofactors considered were infant sex, birth weight, hemoglobin level, and z-scores for growth parameters, and caregiver age, marital status, years of education, number of rooms in the house, and household monthly rent.

Median (50^th percentile) and the interquartile range (IQR) (25^th and 75^th percentiles) for ages at attainment of milestones were calculated using Kaplan-Meier survival methods, with birth as the time origin. Thirty-one (42.5%) HIV-infected infants and 13 (17.3%) HUU infants already had achieved neck control by the time of enrollment, and thus the proportion of infants with neck control by age 5.0 months (the maximum age at enrollment for these 44 infants) was compared. Age at attainment of milestones was compared between groups using log-rank tests for all other milestones. Using this approach, infants who never achieved a given milestone contributed to the analysis until they were censored.

In exploratory analyses, infants with combined 6-month immune and viral responses to ART were compared with HUU infants. For each of these stratified analyses, ages of attainment of walking unsupported and speech for HIV-infected infants with poor immune, virologic, or growth responses, or combined poor immune and virologic responses were also compared with that for HUU infants. In addition, exploratory analyses compared age at speech in infants who received LPV/r-based ART compared with HUU infants.

Statistical analyses were performed using Stata SE, version 11.2, College Station, TX.

Ninety-nine HIV-infected infants were enrolled, of whom 26 died, were lost-to-follow-up or withdrew before initiating ART and providing milestone data, leaving 73 for these analyses [20] (see Additional file 1: Figure S1). Among 100 enrolled HUU infants, seven were lost-to-follow-up or withdrew prior to providing milestone data, and one was diagnosed with cerebral palsy and was excluded from analysis. At enrollment, HIV-infected infants were older than HUU infants (medians, 3.7 vs 1.6 months; P < 0.0001) (Table 1). HIV-infected infants had lower birth weight (3.1 vs 3.2 kg) P = 0.02), and baseline WAZ (medians, −2.0 vs −0.2; P < 0.0001), HAZ (medians, −1.9, vs −1.4; P = 0.04), WHZ (medians, −0.6, vs 1.4; P < 0.0001), and HCZ (medians, −0.5 vs 0.4; P = 0.0002) compared with HUU infants. HIV-infected infants had a median CD4 percentage of 18%, 30 (41.1%) were diagnosed with WHO Stage 3 or 4 disease, and 38 (52.1%) had been hospitalized prior to enrollment. Sixty-two of seventy-three (84.9%) infants had a CD4 percentage below 25%, were diagnosed with WHO Stage 3 or 4 HIV disease, or both, before starting ART.

The majority of HIV-infected infants (97.3%) and (per eligibility criteria) all HUU infants were cared for by their biological mother. The majority of caregivers in each group of infants were married (78.1% vs 87.9%; P = 0.09). Both groups had similar education levels (medians, 9 vs 9 years; P = 0.3), but HIV-infected had lower monthly rent levels (medians, 1,500 vs 2,500 KES; P < 0.0001). The majority of infants in each group lived in a one-room house (76.7% vs 82.4%; P = 0.4).

We previously reported that prior history of hospitalization, a WHO Stage 3 or 4 diagnosis, lower WAZ, HAZ, and WHZ and lower maternal CD4 count were associated with later age at milestone attainment in HIV-infected infants [19]. In the present analysis, HUU infants living in a house with >1 room had earlier age at attainment of milestones (speech, medians, 11 (IQR, 9, 12) vs 12 (IQR, 11, 13) months; P = 0.02; throwing toys, medians, 14 (IQR, 13, 15) vs 15 (IQR 14, 16) months; P = 0.02). Infants living in households with higher rent (>1500 KES/month) also had earlier age at throwing toys (medians, 14 (IQR, 14, 16); vs 17 (IQR, 15, 18) months; P = 0.02).

We hypothesized that HIV-infected infants would have later milestone attainment compared with HUU infants. In Kaplan-Meier analyses, 82.8% (95% CI, 72.9, 90.6) of HIV-infected and 96.6% (95% CI, 91.2, 99.1) of HUU infants had neck control by 5 months of age. HIV-infected infants also had significantly later age at sitting unsupported (medians, 7 vs 6 months; P < 0.0001), walking unsupported (medians, 15 vs 13 months; P < 0.0001) and speech (medians, 15 months vs 12; P = 0.0001), compared with HUU infants (Table 2). Age at attainment of other milestones, including sitting with support, walking with support, and throwing toys were also significantly later compared with HUU. Median age at naming objects was marginally later for HIV-infected and HUU infants, though this did not reach statistical significance (22 versus 19 months; (P = 0.07).

At 6 months post-ART start, 28/54 (51.8%) of infants had viral suppression (plasma HIV RNA <1000 copies/ml), 27 (50.0%) had immune reconstitution (CD4% ≥25), and 38 (70.4%) infants had achieved a WAZ ≥ −2. As would be expected based on prior studies [13, 24], HIV-infected infants with poor 6-month viral responses to ART (plasma HIV RNA ≥1000 copies/ml) had significantly later speech and walking unsupported milestones than HUU infants (all P-values ≤0.0001; Table 3 and Fig. 1). These differences remained significant in analyses adjusted for 6 month post-ART growth (WAZ < −2) and household rent, (all P-values <0.005). Results were similar for infants with poor immune response to ART and underweight (WAZ < −2) at 6-months following start of ART.

We hypothesized that infants with effective responses to ART (defined by their virologic, immune or growth responses) would have significant developmental differences compared with HUU infants. HIV-infected infants with viral suppression had delayed walking unsupported and speech compared to HUU (walking median delay, 2 months; P = 0.0009; speech median delay, 3 months; P <0.0001).

In Cox proportional hazards models adjusted for 6 month post-ART growth status (WAZ < −2) and household rent, infants with viral suppression had significantly later speech (adjusted hazard ratio (aHR), 0.28, 95% confidence interval (CI), 0.16, 0.46; P < 0.001) and a trend to later walking unsupported (aHR, 0.58, 95% CI, 0.36, 0.92; P = 0.02, above the Bonferroni-corrected alpha of 0.008). Infants with 6-month immune reconstitution had delayed speech compared to HUU (aHR, 0.33, 95% CI, 0.21, 0.55; P < 0.001). Infants with sustained WAZ > −2 at 6 months also had later speech (P <0.001). Pre-ART WAZ, 6-month change in WAZ, birth weight, living in a one-room house, and caregiver education were not included in final models due to collinearity. In sensitivity analyses, models adjusted for each of these variables gave similar results.

Eighteen of fifty-four (33.3%) infants had combined viral suppression and immune reconstitution at 6-months post-ART. In exploratory analyses, these infants had similar age at walking unsupported (aHR, 0.73, 95% CI 0.43, 1.26; P = 0.3), but had delayed speech compared with HUU infants (unadjusted median delay, 2 months; P = 0.0002; aHR, 0.40, 95% CI, 0.23, 0.69; P = 0.001). Infants with both poor viral suppression and poor immune reconstitution had even more pronounced delays (walking: median difference delay, 4 months; P = 0.0001; speech delay, 5 months, P < 0.0001) compared with HUU infants. These differences remained in adjusted models (all p-values ≤0.001).

HIV-infected infants in this study received LPV/r-based ART if they had prior exposure to NVP for PMTCT, and we previously reported that infants receiving LPV/r-based ART had significantly earlier speech compared with those receiving NVP-ART [19]. In exploratory analyses, infants receiving LPV/r-based ART still had significantly later speech than HUU infants (aHR, 0.37, 95% CI, 0.21, 0.65; P = 0.001).