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Pathways leading to early growth faltering: an investigation into the importance of mucosal damage and immunostimulation in different socio-economic groups in Nepal

Published online by Cambridge University Press:  29 July 2008

Catherine Panter-Brick*
Affiliation:
Department of Anthropology, Durham University, 43 Old Elvet, DurhamDH1 3HN, UK
Peter G. Lunn
Affiliation:
Department of Biological Anthropology, University of Cambridge, Pembroke street, Cambridge CB2 3DZ, UK
Rebecca M. Langford
Affiliation:
Department of Anthropology, Durham University, 43 Old Elvet, DurhamDH1 3HN, UK
Makhan Maharjan
Affiliation:
Environment and Public Health Organization (ENPHO), 110/124 Adarsa Marg-1, Thapagaon, New Baneshwor, GPO Box 4102, Kathmandu, Nepal
Dharma S. Manandhar
Affiliation:
Mother Infant Research Activities, 755 Prasuti Marg, Thapathali, GPO Box 921, Kathmandu, Nepal
*
*Corresponding author: Professor C. Panter-Brick, fax +44 (0)191 3346101, email catherine.panter-brick@durham.ac.uk
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Abstract

Early childhood growth retardation persists in developing countries despite decades of nutritional interventions. Adequate food is necessary, but not sufficient, to ensure normal growth where there is ubiquitous exposure to infection. Pathways associated with infection, small intestinal mucosal damage and chronic immunostimulation remain largely undemonstrated in countries other than The Gambia. We conducted a longitudinal study of one squatter and one middle-class group (n 86, 3–18 month olds) to assess these relationships in Nepal. Growth, mucosal damage index (MDI; urinary lactose:creatinine ratio adjusted for body weight), morbidity reports, and blood concentrations of albumin, α-1-acid glycoprotein, IgG and Hb, were recorded monthly. Growth status worsened dramatically from 6 to 18 months, with squatters more stunted (height-for-age Z-score (HAZ), P < 0·001) and underweight (weight-for-age Z-score (WAZ), P = 0·009) than middle class. IgG increased with age, was elevated in squatter children, and negatively related to WAZ (P = 0·034). MDI showed significant negative associations with growth performance, explaining 9 and 19 % of height and weight deficits (ΔHAZ, P = 0·004; ΔWAZ, P < 0·001). Unexpectedly, these associations were weaker in squatter children, namely in the group which showed poorer growth, elevated morbidity, greater pathogen exposure (IgG) and higher MDI (P < 0·001). In Nepal, as in The Gambia, children exhibit poor growth, mucosal damage and immunostimulation. The relative impact of pathways associated with infection and undernutrition may, however, differ across socio-economic groups: in poorer children, the impact of mucosal damage and immunostimulation could be masked by nutritional constraints. This has important implications for public health interventions.

Information

Type
Full Papers
Copyright
Copyright © The Authors 2008
Figure 0

Fig. 1 A model of two pathways leading to childhood growth faltering.

Figure 1

Table 1 Demographic and socio-economic characteristics of households in squatter and middle-class groups*

Figure 2

Fig. 2 Reported morbidity levels (7 d recall) for squatter children (■, n 48) and middle-class children (□, n 38). Percentages of reported morbidity each month were averaged across the period of study.

Figure 3

Fig. 3 Growth status for squatter (■) and middle-class (□) children (n 86) in the longitudinal study as Z-scores for height-for-age (a), weight-for-age (b), weight-for-height (c). Values are means with their standard errors depicted by vertical bars.

Figure 4

Fig. 4 Comparison of mucosal damage index (MDI) and plasma protein values for squatter (■) and middle-class (□) children (n 86) for different age bands. (a), MDI; (b), albumin; (c), α-1-acid glycoprotein; (d), Hb; (e), IgG. Values are means with their standard errors depicted by vertical bars.

Figure 5

Table 2 Associations between mucosal damage index and growth status/performance over the period of study*

Figure 6

Fig. 5 Relationships between mucosal damage index (MDI) and growth performance over the period of study. Each point represents the mean MDI and the change in Z-score for an individual child (n 86). (a), Change in height-for-age Z-scores (ΔHAZ): r2 0·09, P = 0·004. (b), Change in weight-for-age Z-scores (ΔWAZ): r2 0·19, P < 0·001.

Figure 7

Table 3 A comparison of anthropometric data, plasma protein concentrations and mucosal damage index (MDI) of age-matched children in Nepal and The Gambia*(Mean values and standard deviations)