Litcius/Paper detail

Chronic UV radiation–induced RORγt+ IL-22–producing lymphoid cells are associated with mutant KC clonal expansion

Julia M. Lewis, Patrick F. Monico, Fatima N. Mirza, Suzanne Xu, Sara Yumeen, Jack L. Turban, Anjela Galan, Michael Girardi

2021Proceedings of the National Academy of Sciences16 citationsDOIOpen Access PDF

Abstract

CCR6+ intracellular CD3+ cutaneous innate lymphoid cell type-3 (ILC3) population (uvILC3) that is associated with UV-induced mutant KC growth. We further show that mutant KC clone size is markedly reduced in the absence of RORγt+ lymphocytes or IL-22, both observed in association with expanding KC clones, and find that topical application of a RORγ/γt inhibitor during chronic UV exposure reduces local expression of IL-22 and IL-17A while markedly limiting mutant p53 KC clonal expansion. We implicate upstream Toll-like receptor signaling in driving this immune response to chronic UV exposure, as MyD88/Trif double-deficient mice also show substantially reduced p53 island number and size. These data elucidate key immune components of chronic UV-induced cutaneous carcinogenesis that might represent targets for skin cancer prevention.

Topics & Concepts

Immune systemSkin cancerCancer researchBiologyRAR-related orphan receptor gammaCancer cellImmunologyCancerFOXP3GeneticsIL-33, ST2, and ILC PathwaysImmune Cell Function and InteractionPsoriasis: Treatment and Pathogenesis