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A TIGIT-based chimeric co-stimulatory switch receptor improves T-cell anti-tumor function.

J Immunother Cancer. 2019; 
Hoogi Shiran,Eisenberg Vasyl,Mayer Shimrit,Shamul Astar,Barliya Tilda,Cohen Cyril
Products/Services Used Details Operation
Catalog Antibody Anti-Vβ12 antibody specific for F4 TCRβ was purchased from Beckman-Coulter/Immunotech (Marseille, France). Biotinylated Protein-L was purchased form Genscript (Piscata, NJ). Get A Quote

摘要

Tumors can employ different mechanisms to evade immune surveillance and function. Overexpression of co-inhibitory ligands that bind to checkpoint molecules on the surface of T-cells can greatly impair the function of latter. TIGIT (T cell immunoreceptor with Ig and ITIM domains) is such a co-inhibitory receptor expressed by T and NK cells which, upon binding to its ligand (e.g., CD155), can diminish cytokine production and effector function. Additionally, the absence of positive co-stimulation at the tumor site can further dampen T-cell response.

关键词

Chimeric receptors,Costimulation,T-cell engineering,TIGIT,Tumor immunothe