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CEACAM1 Activation by CbpF-Expressing

Front Cell Infect Microbiol. 2021-07; 
Amjad Shhadeh, Johanna Galaski, Tamar Alon-Maimon, Jamal Fahoum, Reuven Wiener, Daniel J Slade, Ofer Mandelboim, Gilad Bachrach
Products/Services Used Details Operation
Peptide Synthesis … coli | Cellular and Infection Microbiology … and Infection Microbiology … coli by performing codon optimization (Genscript). In addition to codon optimization, in cbpF-1, the fusobacterial CbpF signal peptide was replaced with that of the E. coli OmpA. … Get A Quote

摘要

Recent studies on the oral, anaerobic, gram-negative bacterium revealed its presence and involvement in colorectal, esophageal and breast cancer. We previously demonstrated that binds and activates the human inhibitory receptors TIGIT and CEACAM1 leading to inhibition of T and NK cell anti-tumor immunity. CEACAM1 was found to be bound and activated by the fusobacterial trimeric autotransporter adhesin CbpF. Here we report the generation of a recombinant expressing full-length CbpF that efficiently binds and activates CEACAM1.

关键词

CEACAM1, CbpF, F. nucleatum, NK cells, trimeric autotransporter adhesin