Anti-human-TIGIT agonistic antibody ameliorates autoimmune diseases by inhibiting Tfh and Tph cells and enhancing Treg cells.
Marenori KojimaKatsuya SuzukiMasaru TakeshitaMasaki OhyagiMana IizukaHumitsugu YamaneKeiko KogaTaku KouroYoshiaki KassaiTomoki YoshiharaRyutaro AdachiKentarou HashikamiYuichiro OtaKeiko YoshimotoYuko KanekoRimpei MoritaAkihiko YoshimuraTsutomu TakeuchiPublished in: Communications biology (2023)
T cells play important roles in autoimmune diseases, but it remains unclear how to optimally manipulate them. We focused on the T cell immunoreceptor with Ig and ITIM domains (TIGIT), a coinhibitory molecule that regulates and is expressed in T cells. In autoimmune diseases, the association between TIGIT-expressing cells and pathogenesis and the function of human-TIGIT (hu-TIGIT) signalling modification have not been fully elucidated. Here we generated anti-hu-TIGIT agonistic monoclonal antibodies (mAbs) and generated hu-TIGIT knock-in mice to accurately evaluate the efficacy of mAb function. Our mAb suppressed the activation of CD4 + T cells, especially follicular helper T and peripheral helper T cells that highly expressed TIGIT, and enhanced the suppressive function of naïve regulatory T cells. These results indicate that our mAb has advantages in restoring the imbalance of T cells that are activated in autoimmune diseases and suggest potential clinical applications for anti-hu-TIGIT agonistic mAbs as therapeutic agents.
Keyphrases
- regulatory t cells
- induced apoptosis
- cell cycle arrest
- dendritic cells
- endothelial cells
- endoplasmic reticulum stress
- cell death
- monoclonal antibody
- immune response
- metabolic syndrome
- oxidative stress
- risk assessment
- cell proliferation
- type diabetes
- insulin resistance
- adipose tissue
- mouse model
- skeletal muscle
- human health