Host tp53 mutation induces gut dysbiosis eliciting inflammation through disturbed sialic acid metabolism.
Jae-Geun LeeSoohyun LeeJuhee JeonHyun Gi KongHyun-Ju ChoJong-Hwan KimSeon-Young KimMyung Jin OhDaum LeeNari SeoKi Hun ParkKweon YuHyun Joo AnChoong Min RyuJeong-Soo LeePublished in: Microbiome (2022)
These results demonstrate a crucial role for host tp53 in maintaining symbiosis and immune homeostasis via SA metabolism. Disturbed SA metabolism via a tp53 mutation may be exploited by specific elements of the gut microbiome, eliciting both dysbiosis and inflammation. Manipulating sialometabolism may therefore provide an efficacious therapeutic strategy for tp53 mutation-induced dysbiosis, inflammation, and ultimately, related cancers. Video Abstract.