Development of nitroalkene-based inhibitors to target STING-dependent inflammation

被引:4
作者
Chang, Fei [1 ]
Gunderstofte, Camilla [2 ]
Colussi, Nicole [1 ]
Pitts, Mareena [3 ]
Salvatore, Sonia R. [1 ]
Thielke, Anne L. [2 ]
Turell, Lucia [4 ,5 ]
Alvarez, Beatriz [4 ,5 ]
Goldbach-Mansky, Raphaela [6 ]
Villacorta, Luis [3 ]
Holm, Christian K. [2 ]
Schopfer, Francisco J. [1 ,7 ,8 ,9 ]
Hansen, Anne Louise [2 ]
机构
[1] Univ Pittsburgh, Dept Pharmacol & Chem Biol, Pittsburgh, PA 15213 USA
[2] Aarhus Univ, Dept Biomed, DK-8000 Aarhus C, Denmark
[3] Morehouse Sch Med, Dept Physiol, Atlanta, GA 30310 USA
[4] Univ Republica, Fac Ciencias, Lab Enzimol, Inst Quim Biol, Montevideo 11400, Uruguay
[5] Univ Republica, Ctr Invest Biomed CEINBIO, Montevideo 11800, Uruguay
[6] NIAID, Translat Autoinflammatory Dis Studies Unit, NIH, Bethesda, MD 20850 USA
[7] Pittsburgh Heart Lung Blood & Vasc Med Inst, Pittsburgh, PA USA
[8] Pittsburgh Liver Res Ctr PLRC, Pittsburgh, PA USA
[9] Ctr Metab & Mitochondrial Med C3M, Pittsburgh, PA USA
关键词
Stimulator of Interferon Genes (STING); Drug discovery; Nitroalkene-based compounds; STING inhibitors; infancy (SAVI); Interferon; NITRO-FATTY ACIDS; CYCLIC GMP-AMP; CONJUGATED LINOLEIC-ACID; DI-GMP; STRUCTURAL BASIS; MURINE MODEL; DNA SENSOR; ACTIVATION; ADAPTER; 2ND-MESSENGER;
D O I
10.1016/j.redox.2024.103202
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Stimulator of Interferon Genes (STING) is essential for the inflammatory response to cytosolic DNA. Despite that aberrant activation of STING is linked to an increasing number of inflammatory diseases, the development of inhibitors has been challenging, with no compounds in the pipeline beyond the preclinical stage. We previously identified endogenous nitrated fatty acids as novel reversible STING inhibitors. With the aim of improving the specificity and efficacy of these compounds, we developed and tested a library of nitroalkene-based compounds for in vitro and in vivo STING inhibition. The structure-activity relationship study revealed a robustly improved electrophilicity and reduced degrees of freedom of nitroalkenes by conjugation with an aromatic moiety. The lead compounds CP-36 and CP-45, featuring a 8-nitrostyrene moiety, potently inhibited STING activity in vitro and relieved STING-dependent inflammation in vivo. This validates the potential for nitroalkene compounds as drug candidates for STING modulation to treat STING-driven inflammatory diseases, providing new robust leads for preclinical development.
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页数:14
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