Associations between Gut Microbiota and Intestinal Inflammation, Permeability and Damage in Young Malawian Children

Author:

Kortekangas Emma1ORCID,Fan Yue-Mei1ORCID,Chaima David2ORCID,Lehto Kirsi-Maarit1,Malamba-Banda Chikondi2,Matchado Andrew23,Chingwanda Chilungamo2,Liu Zhifei1,Ashorn Ulla1,Cheung Yin Bun4ORCID,Dewey Kathryn G3,Maleta Kenneth2ORCID,Ashorn Per15

Affiliation:

1. Center for Child, Adolescent and Maternal Health Research, Faculty of Medicine and Health Technology, Tampere University , Tampere 33014, Finland

2. School of Public Health and Family Medicine, College of Medicine, University of Malawi , Blantyre, Malawi

3. Department of Nutrition and Institute for Global Nutrition, University of California Davis , Davis, CA 95616, USA

4. Program in Health Services & Systems Research and Centre for Quantitative Medicine, Duke-NUS Medical School , Singapore 169857, Singapore

5. Department of Pediatrics, Tampere University Hospital , Tampere 33520, Finland

Abstract

Abstract Background Environmental enteric dysfunction (EED) is common in low- and middle-income countries and associated with childhood undernutrition. The composition of gut microbiota has been implicated in the pathogenesis of EED. Our aim was to assess the associations between gut microbiota and EED biomarkers in rural Malawian children. We hypothesized that there would be an inverse association between microbiota maturity and diversity and fecal concentrations of EED biomarkers. Methods We used data from fecal samples collected at 6, 18 and 30 months from 611 children who were followed up during a nutrition intervention trial. The primary time point for analysis was 18 months. Microbiota data were obtained through 16S rRNA sequencing and variables included microbiota maturity and diversity, phylogenetic dissimilarity and relative abundances of individual taxa. EED biomarkers included calprotectin (marker of inflammation), alpha-1 antitrypsin (intestinal permeability) and REG1B (intestinal damage). Results There was an inverse association between microbiota maturity and diversity and fecal concentrations of all 3 EED biomarkers at 18 months (p≤0.001). The results were similar at 30 months, while at 6 months inverse associations were found only with calprotectin and alpha-1 antitrypsin concentrations. At 18 months, EED biomarkers were not associated with phylogenetic dissimilarity, but at 6 and 30 months several associations were observed. Individual taxa predicting EED biomarker concentrations at 18 months included several Bifidobacterium and Enterobacteriaceae taxa as well as potentially displaced oral taxa. Conclusions Our findings support the hypothesis of an inverse association between microbiota maturity and diversity and EED in rural Malawian children.

Funder

Finnish Funding Agency for Technology and Innovation

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Pediatrics, Perinatology and Child Health

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