Discovery of a selective and biologically active low-molecular weight antagonist of human interleukin-1β

Author:

Hommel UlrichORCID,Hurth KonstanzeORCID,Rondeau Jean-Michel,Vulpetti AnnaORCID,Ostermeier Daniela,Boettcher Andreas,Brady Jacob Peter,Hediger Michael,Lehmann Sylvie,Koch Elke,Blechschmidt Anke,Yamamoto Rina,Tundo Dottorello Valentina,Haenni-Holzinger Sandra,Kaiser Christian,Lehr Philipp,Lingel AndreasORCID,Mureddu Luca,Schleberger ChristianORCID,Blank JuttaORCID,Ramage Paul,Freuler Felix,Eder JoergORCID,Bornancin FrédéricORCID

Abstract

AbstractHuman interleukin-1β (hIL-1β) is a pro-inflammatory cytokine involved in many diseases. While hIL-1β directed antibodies have shown clinical benefit, an orally available low-molecular weight antagonist is still elusive, limiting the applications of hIL-1β-directed therapies. Here we describe the discovery of a low-molecular weight hIL-1β antagonist that blocks the interaction with the IL-1R1 receptor. Starting from a low affinity fragment-based screening hit 1, structure-based optimization resulted in a compound (S)-2 that binds and antagonizes hIL-1β with single-digit micromolar activity in biophysical, biochemical, and cellular assays. X-ray analysis reveals an allosteric mode of action that involves a hitherto unknown binding site in hIL-1β encompassing two loops involved in hIL-1R1/hIL-1β interactions. We show that residues of this binding site are part of a conformationally excited state of the mature cytokine. The compound antagonizes hIL-1β function in cells, including primary human fibroblasts, demonstrating the relevance of this discovery for future development of hIL-1β directed therapeutics.

Funder

RCUK | MRC | Medical Research Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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