posted on 2019-11-18, 20:34authored byRosaura Padilla-Salinas, Rachel Anderson, Kentaro Sakaniwa, Shuting Zhang, Patrick Nordeen, Chuanjun Lu, Toshiyuki Shimizu, Hang Yin
Endosomal toll-like receptors (TLRs) 7 and 8 recognize viral single-stranded RNAs, a class of imidazoquinoline
compounds, 8-oxo-adenosines, 8-aminobenzodiazepines, pyrimidines,
and guanosine analogues. Substantial evidence is present linking chronic
inflammation mediated specifically by TLR7 to the progression of autoimmunity.
We identified a new TLR7/8 dual inhibitor (1) and a TLR8-specific
inhibitor (2) based on our previous screen targeting
TLR8. Compound 1, bearing a benzanilide scaffold, was
found to inhibit TLR7 and TLR8 at low micromolar concentrations. We
envisioned making modifications on the benzanilide scaffold of 1 resulting in a class of highly specific TLR7 inhibitors.
Our efforts led to the discovery of a new TLR8 inhibitor (CU-115) and identification of a TLR7/8 dual inhibitor (CU-72), bearing a distinct diphenyl ether skeleton, with potential for
TLR7 selectivity optimization. Given the role of TLR8 in autoimmunity,
we also optimized the potency of 2 and developed a new
TLR8 inhibitor bearing a 1,3,4-oxadiazole motif.