4.7 Article

Assessment of Environmental Enteric Dysfunction in the SHINE Trial: Methods and Challenges

期刊

CLINICAL INFECTIOUS DISEASES
卷 61, 期 -, 页码 S726-S732

出版社

OXFORD UNIV PRESS INC
DOI: 10.1093/cid/civ848

关键词

infants; stunting; environmental enteric dysfunction; inflammation; IGF-1

资金

  1. Bill & Melinda Gates Foundation [OPP1021542]
  2. Department for International Development, UK
  3. Wellcome Trust, UK [093768/Z/10/Z]
  4. Swiss Agency for Development and Cooperation
  5. US National Institutes of Health [2R01HD060338-06]
  6. European Union

向作者/读者索取更多资源

Environmental enteric dysfunction (EED) is a virtually ubiquitous, but poorly defined, disorder of the small intestine among people living in conditions of poverty, which begins early in infancy and persists. EED is characterized by altered gut structure and function, leading to reduced absorptive surface area and impaired intestinal barrier function. It is hypothesized that recurrent exposure to fecal pathogens and changes in the composition of the intestinal microbiota initiate this process, which leads to a self-perpetuating cycle of pathology. We view EED as a primary gut disorder that drives chronic systemic inflammation, leading to growth hormone resistance and impaired linear growth. There is currently no accepted case definition or gold-standard biomarker of EED, making field studies challenging. The Sanitation Hygiene Infant Nutrition Efficacy (SHINE) trial in Zimbabwe is evaluating the independent and combined effects of a package of infant feeding and/or water, sanitation, and hygiene interventions on stunting and anemia. SHINE therefore provides an opportunity to longitudinally evaluate EED in a well-characterized cohort of infants, using a panel of biomarkers along the hypothesized causal pathway. Our aims are to describe the evolution of EED during infancy, ascertain its contribution to stunting, and investigate the impact of the randomized interventions on the EED pathway. In this article, we describe current concepts of EED, challenges in defining the condition, and our approach to evaluating EED in the SHINE trial.

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