Publication date: Available online 9 August 2018
Source: Clinical Immunology
Author(s): Sabine Hoff, Michiko K. Oyoshi, Jason L. Hornick, Raif S. Geha, NIH/NIAID funded Atopic Dermatitis Research Network
Abstract
Mutations in filaggrin are associated with atopic dermatitis. Filaggrin-deficient flaky tail (Flgft/ft) mice develop spontaneous inflammatory skin lesion that wax and wane. We show that loss of MyD88 promotes the persistence of skin lesions in Flgft/ft mice and exaggerates their expression of the Th17-associated cytokines Il7a and Il22. The development and persistence of skin lesions in Flgft/ft mice was independent of the microbiota. MyD88-mediated signals are shown to be important for the accumulation of T regulatory cells (Tregs) in lesional skin of Flgft/ft mice. Adoptive transfer of WT Tregs dampened the severity of skin lesions in MyD88−/−/Flgft/ft mice. These results suggest that MyD88 signaling in Treg cells by endogenous ligands attenuates skin inflammation in filaggrin deficiency.
https://ift.tt/2nqVugd
Δεν υπάρχουν σχόλια:
Δημοσίευση σχολίου