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Pharmacophore guided discovery of small-molecule interleukin 15 inhibitors

Autor
Niewieczerzał, Szymon
Koziak, Katarzyna
Żyżyńska-Granica, Barbara
Zegrocka-Stendel, Oliwia
Dutkiewicz, Małgorzata
Filipek, Sławomir
Krzeczyński, Piotr
Trzaskowski, Bartosz
Kowalewska, Magdalena
Data publikacji
2017
Abstrakt (EN)

Upregulation of interleukin 15 (IL-15) contributes directly i.a. to the development of inflammatory and autoimmune diseases. Selective blockade of IL-15 aimed to treat rheumatoid arthritis, psoriasis and other IL-15-related disorders has been recognized as an efficient therapeutic method. The aim of the study was to identify small molecules which would interact with IL-15 or its receptor IL-15Rα and inhibit the cytokine's activity. Based on the crystal structure of IL-15Rα·IL-15, we created pharmacophore models to screen the ZINC database of chemical compounds for potential IL-15 and IL-15Rα inhibitors. Twenty compounds with the highest predicted binding affinities were subjected to in vitro analysis using human peripheral blood mononuclear cells to validate in silico data. Twelve molecules efficiently reduced IL-15-dependent TNF-α and IL-17 synthesis. Among these, cefazolin - a safe first-generation cephalosporin antibiotic - holds the highest promise for IL-15-directed therapeutic applications.

Dyscyplina PBN
nauki chemiczne
Czasopismo
European Journal of Medicinal Chemistry
Tom
136
Strony od-do
543-547
ISSN
0223-5234
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