Abstract
Background & AimsEnvironmental enteric dysfunction (EED) limits the Sustainable Development Goals of improved childhood growth and survival. We applied mucosal genomics to advance our understanding of EED.MethodsThe Study of Environmental Enteropathy and Malnutrition (SEEM) followed 416 children from birth to 24 months in a rural district in Pakistan. Biomarkers were measured at 9 months and tested for association with growth at 24 months. The duodenal methylome and transcriptome were determined in 52 undernourished SEEM participants and 42 North American controls and patients with celiac disease.ResultsAfter accounting for growth at study entry, circulating insulin-like growth factor-1 (IGF-1) and ferritin predicted linear growth, whereas leptin correlated with future weight gain. The EED transcriptome exhibited suppression of antioxidant, detoxification, and lipid metabolism genes, and induction of anti-microbial response, interferon, and lymphocyte activation genes. Relative to celiac disease, suppression of antioxidant and detoxification genes and induction of antimicrobial response genes were EED-specific. At the epigenetic level, EED showed hyper-methylation of epithelial metabolism and barrier function genes, and hypo-methylation of immune response and cell proliferation genes. Duodenal coexpression modules showed association between lymphocyte proliferation and epithelial metabolic genes and histologic severity, fecal energy loss, and wasting (weight-for-length/height Z < -2.0). Leptin was associated with expression of epithelial carbohydrate metabolism and stem cell renewal genes. Immune response genes were attenuated by giardia colonization.ConclusionsChildren with reduced circulating IGF-1 are more likely to experience stunting. Leptin and a gene signature for lymphocyte activation and dysregulated lipid metabolism are implicated in wasting, suggesting new approaches for EED refractory to nutritional intervention.ClinicalTrials.gov, Number: NCT03588013. (https://clinicaltrials.gov/ct2/show/NCT03588013)
Highlights
BACKGROUND & AIMSEnvironmental enteric dysfunction (EED) limits the Sustainable Development Goals of improved childhood growth and survival
Random forest and linear regression models which accounted for initial weight and length identified associations between circulating insulin-like growth factor (IGF)-1, ferritin, and leptin, and future growth
Positive correlations (r > 0.4; P < .001) for biomarkers[16] measured at 9 months of age for the overall cohort were noted between insulin-like growth factor-1 (IGF-1) and leptin, C-reactive protein and alpha-1-acid glycoprotein, and tumor necrosis factor a and IFNg (Supplementary Figure 2)
Summary
Environmental enteric dysfunction (EED) limits the Sustainable Development Goals of improved childhood growth and survival. The EED transcriptome exhibited suppression of antioxidant, detoxification, and lipid metabolism genes, and induction of anti-microbial response, interferon, and lymphocyte activation genes. Suppression of antioxidant and detoxification genes and induction of antimicrobial response genes were EEDspecific. EED showed hypermethylation of epithelial metabolism and barrier function genes, and hypo-methylation of immune response and cell proliferation genes. Duodenal coexpression modules showed association between lymphocyte proliferation and epithelial metabolic genes and histologic severity, fecal energy loss, and wasting (weight-for-length/height Z < -2.0). Leptin was associated with expression of epithelial carbohydrate metabolism and stem cell renewal genes. Leptin and a gene signature for lymphocyte activation and dysregulated lipid metabolism are implicated in wasting, Gastroenterology Vol 160, No 6. Clinical and histological similarities suggest potential shared pathogenesis in the most prevalent enteropathies, celiac disease and EED
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