PLoS Neglected Tropical Diseases (Jan 2020)

A novel histological index for evaluation of environmental enteric dysfunction identifies geographic-specific features of enteropathy among children with suboptimal growth.

  • Ta-Chiang Liu,
  • Kelley VanBuskirk,
  • Syed A Ali,
  • M Paul Kelly,
  • Lori R Holtz,
  • Omer H Yilmaz,
  • Kamran Sadiq,
  • Najeeha Iqbal,
  • Beatrice Amadi,
  • Sana Syed,
  • Tahmeed Ahmed,
  • Sean Moore,
  • I Malick Ndao,
  • Michael H Isaacs,
  • John D Pfeifer,
  • Hannah Atlas,
  • Phillip I Tarr,
  • Donna M Denno,
  • Christopher A Moskaluk

DOI
https://doi.org/10.1371/journal.pntd.0007975
Journal volume & issue
Vol. 14, no. 1
p. e0007975

Abstract

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BackgroundA major limitation to understanding the etiopathogenesis of environmental enteric dysfunction (EED) is the lack of a comprehensive, reproducible histologic framework for characterizing the small bowel lesions. We hypothesized that the development of such a system will identify unique histology features for EED, and that some features might correlate with clinical severity.MethodsDuodenal endoscopic biopsies from two cohorts where EED is prevalent (Pakistan, Zambia) and North American children with and without gluten sensitive enteropathy (GSE) were processed for routine hematoxylin & eosin (H&E) staining, and scanned to produce whole slide images (WSIs) which we shared among study pathologists via a secure web browser-based platform. A semi-quantitative scoring index composed of 11 parameters encompassing tissue injury and response patterns commonly observed in routine clinical practice was constructed by three gastrointestinal pathologists, with input from EED experts. The pathologists then read the WSIs using the EED histology index, and inter-observer reliability was assessed. The histology index was further used to identify within- and between-child variations as well as features common across and unique to each cohort, and those that correlated with host phenotype.ResultsEight of the 11 histologic scoring parameters showed useful degrees of variation. The overall concordance across all parameters was 96% weighted agreement, kappa 0.70, and Gwet's AC 0.93. Zambian and Pakistani tissues shared some histologic features with GSE, but most features were distinct, particularly abundance of intraepithelial lymphocytes in the Pakistani cohort, and marked villous destruction and loss of secretory cell lineages in the Zambian cohort.ConclusionsWe propose the first EED histology index for interpreting duodenal biopsies. This index should be useful in future clinical and translational studies of this widespread, poorly understood, and highly consequential disorder, which might be caused by multiple contributing processes, in different regions of the world.