Maternal common mental disorders and infant development in Ethiopia: the P-MaMiE Birth Cohort

The P-MaMiE study was situated in the demographic surveillance site (DSS) at Butajira, a predominantly rural area of Ethiopia located 130 km south of the capital city Addis Ababa. The DSS is part of the Butajira Rural Health Programme (BRHP) http://​www.​indepth-network.​org/​dss_​site_​profiles/​butajira.​pdf.

The P-MaMiE study sample size was determined to address objectives other than those addressed within this paper. For the study presented in this paper, the sampling frame was restricted to infants who were weighed at birth (n = 555). Birth weight was only measured in sub-districts where a suitable health worker could be identified, as previously reported [23]. However, due to low birth weight coverage in the urban sub-district, infants from this sub-district were subsequently excluded from the study. Babies not weighed within 48 hours of birth were also excluded due to the unreliability of birth weight measurements in this group. Overall, birth weight coverage was 79.7% of the remaining eligible babies (n = 521). Women whose infant had birth weight measured within 48 hours of birth did not differ from those whose baby was measured after 48 hours in terms of levels of maternal CMD or on a number of other important variables, as previously reported [23]. A sub-sample of infants who had been weighed within 48 hours of birth was selected for developmental assessment, stratified by level of exposure to maternal antenatal CMD symptoms (see figure 1). All infants exposed to high levels of antenatal CMD symptoms (≥6 on the Self-Reporting Questionnaire-20 (SRQ) [24]) (n = 68) and a random sub-sample of infants exposed to moderate (SRQ score 2 to 5; n = 95/227) and low (SRQ score 0 or 1; n = 95/260) antenatal CMD symptoms were selected for assessment. The number of infants included in the comparison groups was limited by feasibility considerations.

Ethical approval was obtained from the National Ethical Review Committee for Ethiopia and the Research Ethics Committee of King's College London in the UK. Written, informed consent was obtained. All women were reimbursed for health care costs for themselves and their infant. Those women who were suffering from severe mental disturbance were referred for assessment at the local psychiatric unit in Butajira town.

For all analyses, the data were weighted back according to the reciprocal of the achieved sampling fraction (68/55 for high antenatal CMD exposure, 227/62 for moderate CMD exposure and 260/77 for low CMD exposure) using Stata version 10 [38]. Robust standard errors were calculated to account for weighting. Raw Bayley scores were used in all analyses. The initial analysis strategy was hypothesis-driven, using linear regression to investigate the association between exposures of (1) postnatal maternal CMD and (2) antenatal maternal CMD upon infant developmental outcomes. Maternal CMD was added into the model as a continuous exposure variable (SRQ score) in order to maximise power to detect an effect. For the model including antenatal CMD as primary exposure, birth weight and prolonged labour were conceptualised as potentially lying on a causal pathway from antenatal CMD to child development. Infant undernutrition and illness episodes were considered to be probable mediators of any effect of postnatal CMD on child development. Therefore, these variables were not included as potential confounders but were individually added to the final multivariable model to look for preliminary evidence of a mediating role. The potential role of effect modification was explored by including interaction terms in three separate analyses: maternal CMD x socio-economic status, maternal CMD x infant gender, and maternal CMD x perceived social support.

To explore the possible impact of persistent (chronic) maternal CMD, two composite variables were created using the SRQ score cut-off of ≥6 to indicate high levels of CMD symptoms, as supported by our validation study [28]. 'Persistent perinatal CMD' was defined as high CMD in pregnancy and at 2 months postnatal. 'Persistent maternal CMD' was defined as CMD at 2 and 12 months postnatal. Multivariable linear regression analyses were then conducted as above.

Subsequently, an exploratory analysis was conducted to identify the range of variables associated with infant development in this setting. All potential predictors of infant development were included in the final fully adjusted model regardless of whether they were associated in bivariate analyses.

Table 1 shows the background characteristics of participating women and their infants.

At 12 months of age, the prevalence of infants who were underweight (<-2 for Weight-for-Age Z-score) was 41 (21.6%) and 86 (45.5%) were stunted (<-2 for Height-for-Age Z-score).

Only 14 (7.3%) of women had persistent perinatal CMD (SRQ ≥ 6 in pregnancy and at 2 months postnatal), 42 (21.9%) had CMD at either of the perinatal time-points and 139 (70.8%) did not have CMD at either perinatal time-point. In the first postnatal year, 8 (4.1%) of women had persistent maternal CMD (present at both 2 and 12 months postnatal), 18 (9.3%) had CMD at only one postnatal time-point, and 168 (86.6%) did not have CMD at either postnatal time-point.

The mean scores (SD) for the sub-scales of the Bayley were as follows: cognitive 19.2 (3.30), language 20.4 (3.65) and motor 35.6 (4.88).

In both univariate and multivariable linear regression analyses, no association was found between maternal postnatal CMD symptoms (SRQ score) and any of the Bayley developmental sub-scales. When antenatal CMD symptom score was modelled as the primary exposure, an association was seen with motor developmental scores in the univariate analysis (β ^ -0.20; 95% CI: -0.37 to -0.03), but this became non-significant in the final adjusted model (Table 2).

The association between antenatal CMD symptoms and Bayley motor score appeared to be predominantly confounded by parental characteristics, socio-economic status and marital discord. There was no association between antenatal CMD symptoms and either cognitive or language development. There was no evidence that any effect of antenatal CMD upon developmental outcomes was mediated through infant birth weight or maternal experience of prolonged labour.

None of the interaction terms for maternal CMD x socioeconomic status, CMD x infant gender or CMD x social support were significant (results not shown).

A dose-response relationship was observed between the number of time-points at which the infant was exposed to maternal CMD and scores on the motor developmental scale. For the perinatal period, women with CMD either in pregnancy or at postnatal 2 months had infants with a lower mean motor score (β ^ -0.80; 95%CI -2.24, 0.65), and the mean motor score was even lower for women with CMD at both time-points (β ^ -4.19; 95%CI -8.60, 021); test-for-trend χ²13.08(1), p < 0.001. Similarly, for infants whose mothers had CMD at both 2 and 12 months postnatal (See Table 3). These associations became non-significant in the final adjusted models, although there was little change in the size of the β ^ estimates and the confidence intervals were wide. See Table 3.

In the multivariable analyses, poorer infant performance on the cognitive sub-scale was associated with lower self-ranking of wealth relative to others (β ^ -1.50; 95%CI -2.54, -0.45) and maternal experience of physical assault (β ^ -2.72; 95%CI -4.35, -1.09). Higher infant weight-for-height was associated with better cognitive performance (β ^ 0.50; 95%CI 0.03, 0.98). See Table 4.

For the motor sub-scale, poorer performance was associated with lower perceived relative wealth in the multivariable model (β ^ -2.15; 95%CI -3.53, -0.77). Higher infant weight-for-age was significantly associated with better motor performance (β ^ 0.70; 95%CI 0.17, 1.23). See Table 5.

Given the low levels of health service contact by Ethiopian women of reproductive age, it was necessary that the study be population-based. The longitudinal design enabled consideration of direction of causality and reduced measurement bias. A particular strength of the study is that we were able to control for a range of important confounding variables and to distinguish effects of antenatal, postnatal, and persistent exposure to maternal CMD.

Some potential study limitations need to be borne in mind when interpreting our findings. First, the Western-derived measure of infant development, the Bayley Scales, may not have been culturally valid in this setting. Arguing against this as a major limitation are the previous reports of successful use of the Bayley Scales in Ethiopia [26, 27]. Furthermore, a rigorous attempt to develop a more culturally valid measure of child development in another sub-Saharan African country, by adding new items and discarding those with poor test properties, found that the majority of items from the original Western scale could be adapted for use in the final scale [39]. Further support for the construct validity of the Bayley Scales comes from our finding that developmental scores were associated with expected predictors of developmental outcome. The lack of formal assessment of reliability of administration of the Bayley Scales was a further limitation, although a previous Ethiopian study demonstrated that careful training and monitoring of administrators, as was done in our study, may suffice [27]. Second, the assessment of language development may have been affected by the limited range of language typical of 12 month old infants [40] and by the necessity of relying on mothers' reports.

A third study limitation is the relatively small number of women with high levels of CMD symptoms in our sample, raising the possibility that we were under-powered to detect a true effect of maternal CMD on infant development. Fourth, overadjustment for confounding variables is a possible explanation for our negative finding. This could be a particular problem for variables that could be subject to recall bias, such as maternal and infant illness episodes. However, the lack of significant associations in the crude analyses argues against this as an important factor. Fifth, our use of maternal CMD symptoms as the measure of mental ill-health rather than restricting the exposure to depressive symptoms or a diagnosis of major depressive disorder might have diluted any effect on infant development [41]. However, previous studies relying on symptom scales have shown associations with impaired infant development [8, 21, 29, 42]. Lastly, exploring features of the home environment and, specifically, characteristics of mother-infant interactions and the child-rearing practices of other caregivers would have added useful information on risk and protective factors that might modulate the effect of maternal CMD exposure upon infant development.

Our study findings are inconsistent with the results of a number of studies conducted in high-income countries [4, 8, 11, 29, 40, 42] that have demonstrated adverse effects of maternal CMD, particularly in the postnatal period, upon infant and child cognitive and motor development. However, other well-conducted high-income country studies have either failed to replicate this association [5] or found that early exposure to maternal CMD explains little of the variability of the child developmental outcomes [29] or only detected an association in vulnerable sub-groups [12, 16]. Furthermore, some studies only found an association between maternal CMD and specific cognitive tasks, for example, Piaget's object concept, and not with more global assessments of cognitive functioning [16, 43].

Methodological differences may also go some way to explaining the lack of congruence with findings from previous LAMICs. Samples recruited from health facilities [19] might be biased towards more severe and chronic cases of maternal CMD. In the only other rural, prospective population-based study, based in Bangladesh [22], maternal CMD was not independently associated with infant development. The previous Ethiopian study was limited by the cross-sectional design and use of a non-validated measure of maternal CMD which may have led to measurement bias [21]. Differences in the timing of assessment of maternal CMD and infant development further complicate comparisons among studies. Later measurement of cognitive function may show the effects of maternal perinatal mental health more clearly [20].

Again contrary to some other studies from LAMICs [44], we have previously demonstrated a lack of association between maternal CMD and birthweight [23] and infant undernutrition [45] in this rural Ethiopian population. As infant undernutrition is an important risk factor for impaired development [1], this may explain the observed lack of association between maternal CMD and child development. Protective factors may prevent the negative consequences of risk factors upon infant development by influencing mediating factors; for example, mother-infant interaction, maternal cognition or characteristics of the home environment [46]. In this regard it is interesting to observe that available data on child-rearing practices in the sample population show that, although mothers are the primary care givers for the majority of infants, in a third of cases older siblings look after the infants for the longest time per day. Further exploration of potentially protective socio-cultural factors in the home environment and local community which may buffer negative effects of maternal mental health on infant development is indicated.

Although limited by the small numbers of women with persistent CMD in our study, there was some evidence to support an effect of chronicity of maternal CMD upon motor development. Univariate analyses found statistically significant associations, with little change in the size of the beta-coefficients when adjusting for a broad range of confounders; however, in the final adjusted model the confidence intervals were wide, rendering the result non-significant. The importance of distinguishing between mild and transient perinatal depressive symptoms and chronic mental disorders has been demonstrated in several studies, with effects on child development only seen with more enduring maternal mental disorder [8, 29, 40].

Our finding that perceived lower relative wealth is associated with poorer infant cognitive and motor development is in keeping with previous studies [15]. Similarly, poor infant nutritional status (stunting and under-weight) is an established risk factor for both cognitive and motor developmental delay [1]. This association has also been confirmed in three previous Ethiopian studies [21, 26, 27]. A growing body of evidence supports the importance of interpersonal violence during pregnancy for infant outcomes [47]. In our study, the effect of physical violence on infant cognitive outcome is unlikely to have been mediated through low birth weight as we were able to adjust for this in the multivariable analysis. A more probable explanation is continuity of violence from pregnancy into the postnatal period so that the developing child is exposed to the detrimental effects of ongoing family conflict [11].

Our findings support the need to build capacity of primary health care workers providing ante- and postnatal services in LAMICs to identify mothers exposed to risk factors that may affect child development, particularly social adversity and violence. Psychosocial interventions to improve child development have already been successfully trialled in a sub-Saharan Africa setting [48]. The P-MaMiE cohort is continuing to be followed up with further assessments of child development in relation to maternal mental health, providing an opportunity to investigate the impact of chronicity of maternal CMD beyond the perinatal period. Exploration of potential protective factors that may contribute to infants' resilience to maternal CMD is also indicated.