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An epithelial <i>Nfkb2</i> pathway exacerbates intestinal inflammation by supplementing latent RelA dimers to the canonical NF-κB module

M. L. Chawla, Tapas Mukherjee, Alvina Deka, Budhaditya Chatterjee, Uday Aditya Sarkar, Amit Singh, Saurabh Kedia, Josephine Lum, Manprit Kaur Dhillon, Balaji Banoth, Subhra K. Biswas, Vineet Ahuja, Soumen Basak

2021Proceedings of the National Academy of Sciences61 citationsDOIOpen Access PDF

Abstract

Significance The canonical NF-κB pathway mediates controlled nuclear activation of RelA factors, which induce proinflammatory genes. Uncontrolled RelA activity, however, fuels aberrant intestinal inflammation. What triggers pathological RelA activity in the colitogenic gut remains unclear. The noncanonical NF-κB module typically directs immune organogenesis involving Nfkb2 gene products. We find that this otherwise harmless noncanonical signaling amplifies canonical RelA activity in the inflamed colon in inflammatory bowel disease patients and in colitogenic mice, aggravating gut pathologies. Our work further suggests that noncanonical signaling supplements copious amounts of RelA dimers, whose activation by canonical signaling exacerbates gut inflammation. In sum, we reveal a mechanism regulating disease-associated inflammation and present the noncanonical Nfkb2 pathway as an attractive therapeutic option in inflammatory diseases.

Topics & Concepts

InflammationProinflammatory cytokineNF-κBInflammatory bowel diseaseNFKB1Cell biologyImmunologySignal transductionBiologyCancer researchDiseaseGeneMedicineTranscription factorGeneticsInternal medicineNF-κB Signaling PathwaysHelicobacter pylori-related gastroenterology studiesImmune Response and Inflammation
An epithelial <i>Nfkb2</i> pathway exacerbates intestinal inflammation by supplementing latent RelA dimers to the canonical NF-κB module | Litcius