3PO inhibits inflammatory NF[kappa]B and stress-activated kinase signaling in primary human endothelial cells independently of its target PFKFB3

3PO inhibits inflammatory NF[kappa]B and stress-activated kinase signaling in primary human endothelial cells independently of its target PFKFB3

Inhibition of the key glycolytic activator 6-phosphofructokinase 2/fructose-2,6-bisphosphatase-3 (PFKFB3) by 3-(3-pyridinyl)-1-(4-pyridinyl)-2-propen-1-one (3PO) strongly attenuates pathological angiogenesis in cancer and inflammation. In addition to modulating endothelial proliferation and migratio...

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Veröffentlicht in:PloS one 2020-03, Vol.15 (3), p.e0229395
Hauptverfasser: Wik, Jonas Aakre, Lundbäck, Peter, la Cour Poulsen, Lars, Haraldsen, Guttorm, Skålhegg, Bjørn Steen, Hol, Johanna
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Anti-inflammatory agents
EDTA
Endothelium
Fructose
Glucose metabolism
Inflammation
Monosaccharides
Scientific equipment industry
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container_issue 3
container_start_page e0229395
container_title PloS one
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creator Wik, Jonas Aakre
Lundbäck, Peter
la Cour Poulsen, Lars
Haraldsen, Guttorm
Skålhegg, Bjørn Steen
Hol, Johanna
description Inhibition of the key glycolytic activator 6-phosphofructokinase 2/fructose-2,6-bisphosphatase-3 (PFKFB3) by 3-(3-pyridinyl)-1-(4-pyridinyl)-2-propen-1-one (3PO) strongly attenuates pathological angiogenesis in cancer and inflammation. In addition to modulating endothelial proliferation and migration, 3PO also dampens proinflammatory activation of endothelial cells and experimental inflammation in vivo, suggesting a potential for 3PO in the treatment of chronic inflammation. The aim of our study was to explore if the anti-inflammatory action of 3PO in human endothelial cells was mediated by inhibition of PFKFB3 and glycolysis and assess if other means of PFKFB3 inhibition reduced inflammatory activation in a similar manner. We found that 3PO caused a rapid and transient reduction in IL-1[beta]- and TNF-induced phosphorylation of both IKK[alpha]/[beta] and JNK, thus inhibiting signaling through the NF[kappa]B and the stress-activated kinase pathways. However, in contrast to 3PO-treatment, neither shRNA-mediated silencing of PFKFB3 nor treatment with the alternative PFKFB3 inhibitor 7,8-dihydroxy-3-(4-hydroxy-phenyl)-chromen-4-one (YN1) prevented cytokine-induced NF[kappa]B signaling and upregulation of the adhesion molecules VCAM-1 and E-selectin, implying off target effects of 3PO. Collectively, our results suggest that the anti-inflammatory action of 3PO in human endothelial cells is not limited to inhibition of PFKFB3 and cellular glycolysis.
doi_str_mv 10.1371/journal.pone.0229395
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In addition to modulating endothelial proliferation and migration, 3PO also dampens proinflammatory activation of endothelial cells and experimental inflammation in vivo, suggesting a potential for 3PO in the treatment of chronic inflammation. The aim of our study was to explore if the anti-inflammatory action of 3PO in human endothelial cells was mediated by inhibition of PFKFB3 and glycolysis and assess if other means of PFKFB3 inhibition reduced inflammatory activation in a similar manner. We found that 3PO caused a rapid and transient reduction in IL-1[beta]- and TNF-induced phosphorylation of both IKK[alpha]/[beta] and JNK, thus inhibiting signaling through the NF[kappa]B and the stress-activated kinase pathways. 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subjects Anti-inflammatory agents
EDTA
Endothelium
Fructose
Glucose metabolism
Inflammation
Monosaccharides
Scientific equipment industry
title 3PO inhibits inflammatory NF[kappa]B and stress-activated kinase signaling in primary human endothelial cells independently of its target PFKFB3
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