Pyridazinones and Structurally Related Derivatives with Anti-Inflammatory Activity

Niccolo Cantini; Igor A. Schepetkin; Nadezhda V. Danilenko; Andrei I. Khlebnikov; Letizia Crocetti; Maria Paola Giovannoni; Liliya N. Kirpotina; Mark T. Quinn

doi:10.3390/molecules27123749

Molecules (Jun 2022)

Pyridazinones and Structurally Related Derivatives with Anti-Inflammatory Activity

Niccolo Cantini,
Igor A. Schepetkin,
Nadezhda V. Danilenko,
Andrei I. Khlebnikov,
Letizia Crocetti,
Maria Paola Giovannoni,
Liliya N. Kirpotina,
Mark T. Quinn

Affiliations

Niccolo Cantini: Department of Microbiology and Cell Biology, Montana State University, Bozeman, MT 59717, USA
Igor A. Schepetkin: Department of Microbiology and Cell Biology, Montana State University, Bozeman, MT 59717, USA
Nadezhda V. Danilenko: Kizhner Research Center, Tomsk Polytechnic University, Tomsk 634050, Russia
Andrei I. Khlebnikov: Kizhner Research Center, Tomsk Polytechnic University, Tomsk 634050, Russia
Letizia Crocetti: NEUROFARBA, Pharmaceutical and Nutraceutical Section, University of Florence, 50019 Sesto Fiorentino, Italy
Maria Paola Giovannoni: NEUROFARBA, Pharmaceutical and Nutraceutical Section, University of Florence, 50019 Sesto Fiorentino, Italy
Liliya N. Kirpotina: Department of Microbiology and Cell Biology, Montana State University, Bozeman, MT 59717, USA
Mark T. Quinn: Department of Microbiology and Cell Biology, Montana State University, Bozeman, MT 59717, USA

DOI: https://doi.org/10.3390/molecules27123749
Journal volume & issue: Vol. 27, no. 12
p. 3749

Abstract

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Persistent inflammation contributes to a number of diseases; therefore, control of the inflammatory response is an important therapeutic goal. In an effort to identify novel anti-inflammatory compounds, we screened a library of pyridazinones and structurally related derivatives that were used previously to identify N-formyl peptide receptor (FPR) agonists. Screening of the compounds for their ability to inhibit lipopolysaccharide (LPS)-induced nuclear factor κB (NF-κB) transcriptional activity in human THP1-Blue monocytic cells identified 48 compounds with anti-inflammatory activity. Interestingly, 34 compounds were FPR agonists, whereas 14 inhibitors of LPS-induced NF-κB activity were not FPR agonists, indicating that they inhibited different signaling pathways. Further analysis of the most potent inhibitors showed that they also inhibited LPS-induced production of interleukin 6 (IL-6) by human MonoMac-6 monocytic cells, again verifying their anti-inflammatory properties. Structure–activity relationship (SAR) classification models based on atom pair descriptors and physicochemical ADME parameters were developed to achieve better insight into the relationships between chemical structures of the compounds and their biological activities, and we found that there was little correlation between FPR agonist activity and inhibition of LPS-induced NF-κB activity. Indeed, Cmpd43, a well-known pyrazolone-based FPR agonist, as well as FPR1 and FPR2 peptide agonists had no effect on the LPS-induced NF-κB activity in THP1-Blue cells. Thus, some FPR agonists reported to have anti-inflammatory activity may actually mediate their effects through FPR-independent pathways, as it is suggested by our results with this series of compounds. This could explain how treatment with some agonists known to be inflammatory (i.e., FPR1 agonists) could result in anti-inflammatory effects. Further research is clearly needed to define the molecular targets of pyridazinones and structurally related compounds with anti-inflammatory activity and to define their relationships (if any) to FPR signaling events.

Published in Molecules

ISSN: 1420-3049 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Chemistry: Organic chemistry
Website: http://www.mdpi.com/journal/molecules

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