| Literature DB >> 30954385 |
Qiao Su1, Jun Jing2, Wuguo Li1, Jianda Ma2, Xueling Zhang1, Zongren Wang3, Zhongyang Zhou1, Lie Dai4, Lan Shao5.
Abstract
In rheumatoid arthritis (RA), imbalanced T cells subsets play a critical role in sustaining chronic inflammatory responses in the synovium. Naïve T cells in RA patients undergo maldifferentiation, including an increase in the effector Th1/Th17 lineage and a reduction in regulatory T (Treg) cells. Upon stimulation, naïve CD4+CD45RO- T cells from RA patients exhibited insufficient expression of Foxp3, which induced a deficiency in Tregs production and an imbalance of Treg/Th17 differentiation. Further mechanistic study indicated that RA T cells failed to produce sufficient levels of the histone acetyltransferase Tip60, leading to reduced acetylation of Foxp3; this, in turn, decreased Foxp3 expression, impaired Treg commitment, and promoted Th17 production. Moreover, in human synovium chimeric mice, suppression of Tip60 activity in healthy T cells promoted tissue infiltration and arthritogenesis, while reconstitution of Tip60 in RA T cells suppressed synovitis and effector T cell infiltration. Our findings link T cell maldifferentiation and tissue infiltration with Tip60-mediated Foxp3 acetylation and identify Tip60 as a potential therapeutic target for suppression of tissue inflammation and autoimmunogenesis in RA.Entities:
Keywords: Acetylation; Foxp3; Rheumatoid arthritis; T cell differentiation; Tip60
Year: 2019 PMID: 30954385 DOI: 10.1016/j.jaut.2019.02.007
Source DB: PubMed Journal: J Autoimmun ISSN: 0896-8411 Impact factor: 7.094