FOXO inhibition rescues α-defensin expression in human intestinal organoids

To mediate critical host-microbe interactions in the human small intestine, Paneth cells constitutively produce abundant levels of α-defensins and other antimicrobials. We report that the expression profile of these antimicrobials is dramatically askew in human small intestinal organoids (enteroids)...

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Veröffentlicht in:Proceedings of the National Academy of Sciences - PNAS 2023-11, Vol.120 (47), p.e2312453120-e2312453120
Hauptverfasser: Eng, Serena J, Nonnecke, Eric B, de Lorimier, Arthur J, Ali, Mohamed R, Tsolis, Renée M, Bevins, Charles L, Ashwood, Paul
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Sprache:eng
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Zusammenfassung:To mediate critical host-microbe interactions in the human small intestine, Paneth cells constitutively produce abundant levels of α-defensins and other antimicrobials. We report that the expression profile of these antimicrobials is dramatically askew in human small intestinal organoids (enteroids) as compared to that in paired tissue from which they are derived, with a reduction of α-defensins to nearly undetectable levels. Murine enteroids, however, recapitulate the expression profile of Paneth cell α-defensins seen in tissue. WNT/TCF signaling has been found to be instrumental in the regulation of α-defensins, yet in human enteroids exogenous stimulation of WNT signaling appears insufficient to rescue α-defensin expression. By stark contrast, forkhead box O (FOXO) inhibitor AS1842856 induced the expression of α-defensin mRNA in enteroids by >100,000-fold, restoring and to levels comparable to those found in primary human tissue. These results newly identify FOXO signaling as a pathway of biological and potentially therapeutic relevance for the regulation of human Paneth cell α-defensins in health and disease.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.2312453120