Small Molecule IL-36γ Antagonist as a Novel Therapeutic Approach for Plaque Psoriasis

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作者
Viktor Todorović
Zhi Su
C. Brent Putman
Stevan J. Kakavas
Katherine M. Salte
Heath A. McDonald
Joseph B. Wetter
Stephanie E. Paulsboe
Qi Sun
Clare E. Gerstein
Limary Medina
Bernhard Sielaff
Ramkrishna Sadhukhan
Henning Stockmann
Paul L. Richardson
Wei Qiu
Maria A. Argiriadi
Rodger F. Henry
J. Martin Herold
J. Brad Shotwell
Steve P. McGaraughty
Prisca Honore
Sujatha M. Gopalakrishnan
Chaohong C. Sun
Victoria E. Scott
机构
[1] AbbVie Inc.,
[2] AbbVie Bioresearch Center,undefined
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Scientific Reports | / 9卷
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摘要
IL-36 cytokines are pro-inflammatory members of the IL-1 family that are upregulated in inflammatory disorders. Specifically, IL-36γ is highly expressed in active psoriatic lesions and can drive pro-inflammatory processes in 3D human skin equivalents supporting a role for this target in skin inflammation. Small molecule antagonists of interleukins have been historically challenging to generate. Nevertheless, we performed a small molecule high-throughput screen to identify IL-36 antagonists using a novel TR-FRET binding assay. Several compounds, including 2-oxypyrimidine containing structural analogs of the marketed endothelin receptor A antagonist Ambrisentan, were identified as hits from the screen. A-552 was identified as a the most potent antagonist of human IL-36γ, but not the closely related family member IL-36α, was capable of attenuating IL-36γ induced responses in mouse and human disease models. Additionally, x-ray crystallography studies identified key amino acid residues in the binding pocket present in human IL-36γ that are absent in human IL-36α. A-552 represents a first-in-class small molecule antagonist of IL-36 signaling that could be used as a chemical tool to further investigate the role of this pathway in inflammatory skin diseases such as psoriasis.
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