4.7 Article

Commensal Bacteria Modulate Immunoglobulin A Binding in Response to Host Nutrition

Journal

CELL HOST & MICROBE
Volume 27, Issue 6, Pages 909-+

Publisher

CELL PRESS
DOI: 10.1016/j.chom.2020.03.012

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Funding

  1. Canadian Institutes of Health Research (CIHR)
  2. Bill and Melinda Gates Foundation
  3. CIHR
  4. Killam

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Immunoglobulin (Ig) A controls host-microbial homeostasis in the gut. IgA recognition of beneficial bacteria is decreased in acutely undernourished children, but the factors driving these changes in IgA targeting are unknown. Child undernutrition is a global health challenge that is exacerbated by poor sanitation and intestinal inflammation. To understand how nutrition impacts immune-microbe interactions, we used a mouse model of undernutrition with or without fecal-oral exposure and assessed IgA-bacterial targeting from weaning to adulthood. In contrast to healthy control mice, undernourished mice fail to develop IgA recognition of intestinal Lactobacillus. Glycan-mediated interactions between Lactobacillus and host antibodies are lost in undernourished mice due to rapid bacterial adaptation. Lactobacillus adaptations occur in direct response to nutritional pressure, independently of host IgA, and are associated with reduced mucosal colonization and with bacterial mutations in carbohydrate processing genes. Together these data indicate that diet-driven bacterial adaptations shape IgA recognition in the gut.

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