4.7 Article

Mechanism of iron on the intestinal epithelium development in suckling piglets

Journal

SCIENCE CHINA-LIFE SCIENCES
Volume 66, Issue 9, Pages 2070-2085

Publisher

SCIENCE PRESS
DOI: 10.1007/s11427-022-2307-7

Keywords

iron; suckling piglets; intestinal epithelium development; interleukin-22

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This study investigated the effect of iron on intestinal epithelium development in suckling piglets. The results showed that lactation is a critical stage for intestinal epithelial development and is associated with changes in iron metabolism. Iron deficiency does not directly affect intestinal epithelium development through intestinal stem cells, but IL-22 may play a key role in this process.
This study aimed to investigate the mechanism of iron on intestinal epithelium development of suckling piglets. Compared with newborn piglets, 7-day-old and 21-day-old piglets showed changes in the morphology of the jejunum, increased proliferation, differentiated epithelial cells, and expanded enteroids. Intestinal epithelium maturation markers and iron metabolism genes were significantly changed. These results suggest that lactation is a critical stage in intestinal epithelial development, accompanied by changes in iron metabolism. In addition, deferoxamine (DFO) treatment inhibited the activity of intestinal organoids at passage 4 (P4) of 0-day-old piglets, but no significant difference was observed in epithelial maturation markers at passage 1 (P1) and P4, and only argininosuccinate synthetase 1 (Ass1) and beta-galactosidase (Gleb) were up-regulated at passage 7 (P7). These results in vitro show that iron deficiency may not directly affect intestinal epithelium development through intestinal stem cells (ISCs). The iron supplementation significantly down-regulated the mRNA expression of interleukin-22 receptor subunit alpha-2 (IL-22RA2) in the jejunum of piglets. Furthermore, the mRNA expression of IL-22 in 7-day-old piglets was significantly higher than that in 0-day-old piglets. Adult epithelial markers were significantly up-regulated in organoids treated with recombinant murine cytokine IL-22. Thus, IL-22 may play a key role in iron-affecting intestinal epithelium development.

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