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. 2023 Apr;24(4):585-594.
doi: 10.1038/s41590-023-01450-z. Epub 2023 Mar 20.

Epithelial Nlrp10 inflammasome mediates protection against intestinal autoinflammation

Danping Zheng #  1   2 Gayatree Mohapatra #  1 Lara Kern #  1 Yiming He  1   2 Merav D Shmueli  1 Rafael Valdés-Mas  1 Aleksandra A Kolodziejczyk  1 Tomasz Próchnicki  3 Matilde B Vasconcelos  3 Lena Schorr  4   5 Franziska Hertel  4 Ye Seul Lee  4 Miguel Camacho Rufino  1 Emmanuelle Ceddaha  1 Sandy Shimshy  1 Ryan James Hodgetts  1   6 Mally Dori-Bachash  1 Christian Kleimeyer  1 Kim Goldenberg  1 Melina Heinemann  1 Noa Stettner  7 Alon Harmelin  7 Hagit Shapiro  1 Jens Puschhof  4 Minhu Chen  2 Richard A Flavell  8   9 Eicke Latz  3 Yifat Merbl  1 Suhaib K Abdeen  10 Eran Elinav  11   12
Affiliations

Epithelial Nlrp10 inflammasome mediates protection against intestinal autoinflammation

Danping Zheng et al. Nat Immunol. 2023 Apr.

Abstract

Unlike other nucleotide oligomerization domain-like receptors, Nlrp10 lacks a canonical leucine-rich repeat domain, suggesting that it is incapable of signal sensing and inflammasome formation. Here we show that mouse Nlrp10 is expressed in distal colonic intestinal epithelial cells (IECs) and modulated by the intestinal microbiome. In vitro, Nlrp10 forms an Apoptosis-associated speck-like protein containing a caspase-recruitment domain (ASC)-dependent, m-3M3FBS-activated, polyinosinic:polycytidylic acid-modulated inflammasome driving interleukin-1β and interleukin-18 secretion. In vivo, Nlrp10 signaling is dispensable during steady state but becomes functional during autoinflammation in antagonizing mucosal damage. Importantly, whole-body or conditional IEC Nlrp10 depletion leads to reduced IEC caspase-1 activation, coupled with enhanced susceptibility to dextran sodium sulfate-induced colitis, mediated by altered inflammatory and healing programs. Collectively, understanding Nlrp10 inflammasome-dependent and independent activity, regulation and possible human relevance might facilitate the development of new innate immune anti-inflammatory interventions.

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Comment in

  • Ten things to know about NLRP10.
    Masters SL. Masters SL. Nat Immunol. 2023 Apr;24(4):561-562. doi: 10.1038/s41590-023-01466-5. Nat Immunol. 2023. PMID: 36949288 No abstract available.

References

    1. Franchi, L., Warner, N., Viani, K. & Nuñez, G. Function of Nod-like receptors in microbial recognition and host defense. Immunol. Rev. 227, 106–128 (2009). - DOI - PubMed - PMC
    1. Strowig, T., Henao-Mejia, J., Elinav, E. & Flavell, R. Inflammasomes in health and disease. Nature 481, 278–286 (2012). - DOI - PubMed
    1. Franchi, L. et al. NLRC4-driven production of IL-1β discriminates between pathogenic and commensal bacteria and promotes host intestinal defense. Nat. Immunol. 13, 449–456 (2012). - DOI - PubMed - PMC
    1. Elinav, E. et al. NLRP6 inflammasome regulates colonic microbial ecology and risk for colitis. Cell 145, 745–757 (2011). - DOI - PubMed - PMC
    1. Zhu, S. et al. Nlrp9b inflammasome restricts rotavirus infection in intestinal epithelial cells. Nature 546, 667–670 (2017). - DOI - PubMed - PMC

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