LGR5 constitutively activates NF‐κB signaling to regulate the growth of intestinal crypts.

Mammalian LGR5 and LGR4, markers of adult stem cells, are involved in many physiological functions by enhancing WNT signaling. However, whether LGR5 and LGR4 are coupled to other intracellular signaling pathways to regulate stem cell function remains unknown. Here, we show that LGR5 and LGR4 can constitutively activate NF‐κB signaling in a ligand‐independent manner, which is dependent on their C‐termini, but independent of receptor endocytosis. Moreover, the C‐termini of LGR5/4 interact with TROY, which is required for activating NF‐κB signaling. In small intestinal crypt organoids, overexpression of a C‐terminal deletion mutant of LGR5 inhibits the growth and bud formation of organoids, whereas overexpression of the R‐spondin‐binding mutant of LGR5 that is defective for WNT signaling can still promote organoid growth. Our study reveals that NF‐κB signaling, regulated by LGR5 and LGR4, plays an important role in the survival of colon cancer cells and the growth of intestinal crypts. Our findings also suggest that LGR5/4‐induced NF‐κB signaling and WNT signaling may co‐regulate the growth of LGR5+ adult stem cells and intestinal crypts. [ABSTRACT FROM AUTHOR]