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Rational design of anti-GITR-based combination immunotherapy.

Nat. Med.. 2019-05; 
ZappasodiRoberta,SirardCynthia,LiYanyun,BudhuSadna,Abu-AkeelMohsen,LiuCailian,YangXia,ZhongHong,NewmanWalter,QiJingjing,WongPhillip,SchaerDavid,KoonHenry,VelchetiVamsidhar,HellmannMatthew D,PostowMichael A,CallahanMargaret K,WolchokJedd D,Merghoub
Products/Services Used Details Operation
Catalog Antibody TRX518 or isotype control or recombinant human GITR ligand (GenScript) (10 µg ml−1) and soluble anti-CD28 (0.1 µg ml−1) in the presence of a fluorogenic caspase 3/7 substrate (1 µM, Invitrogen) for 16 and 32 h. Get A Quote

摘要

Modulating T cell homeostatic mechanisms with checkpoint blockade can efficiently promote endogenous anti-tumor T cell responses. However, many patients still do not benefit from checkpoint blockade, highlighting the need for targeting of alternative immune pathways. Glucocorticoid-induced tumor necrosis factor receptor-related protein (GITR) is an attractive target for immunotherapy, owing to its capacity to promote effector T cell (T) functions and hamper regulatory T cell (T) suppression. On the basis of the potent preclinical anti-tumor activity of agonist anti-GITR antibodies, reported by us and others, we initiated the first in-human phase 1 trial of GITR agonism with the anti-GITR antibody TRX5... More

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