Stimulator of interferon genes (STING) is a transmembrane endoplasmic reticulum (ER) resident protein involved in innate immunity. STING activation occurs by binding of cyclic guanosine-(2'â5')-monophosphate-adenosine-(3'â5')-monophosphate (2',3'-cGAMP) to STING, which leads to downstream production of type 1 interferons (IFN-1). We generated molecular dynamics (MD) equilibrated agonist and antagonist models of human STING (hSTING) for computer-based screening and now report the discovery of clonixeril (CXL) as the most potent non-nucleotide hSTING modulator discovered to date. We demonstrate in vitro and in cellulo that CXL has two modes of interaction with hSTING, one with an EC(50) above 1 nM and the other with an EC(50) in the 1 fM-100 aM range (10(-15)-10(-16) M). In cell-based experiments, when CXL is titrated below 1 nM, it displays inverse dose-dependent antagonistic behavior toward hSTING. We have substantiated that CXL displays this exceptionally strong inhibitory effect on hSTING mediated IFN-1 production using a THP-1 cell luciferase reporter for interferon regulatory factor 3 (IRF3). Further characterization of CXL was performed in HEK293 cells by using biophysical and biochemical techniques.
Discovery of Clonixeril as a Sub-Femtomolar Modulator of the Human STING Receptor.
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作者:Sparks Robert P, Lawless William, Kharitonova Anna, Metcalf Rainer, Nunziata Jamie, Binder Grace A, Chaudhuri Sauradip, Gambino Christine S R, Wilde Michelle, Harding Linette S, Crews Jaret J, Gopu Mansi, Dalamangas Emilia, Lawless Sarah, Eschenfelder Mark, Green Robert M, Nompleggi Elizabeth X, Tran Timothy H, Yang Yan, Trask Donna V, Thompson Paul R, Patel Rekha, Patel Niketa A, Brooks Wesley H, Bradley Guy, Acevedo-Duncan Mildred E, Mullen Alan C, Leahy James W, Daniel Kenyon G, Guida Wayne C
| 期刊: | ACS Central Science | 影响因子: | 10.400 |
| 时间: | 2025 | 起止号: | 2025 Jun 6; 11(6):994-1008 |
| doi: | 10.1021/acscentsci.4c01982 | ||
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