2018
DOI: 10.3390/molecules23081979
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Phosphocholine-Modified Lipooligosaccharides of Haemophilus influenzae Inhibit ATP-Induced IL-1β Release by Pulmonary Epithelial Cells

Abstract: Phosphocholine-modified bacterial cell wall components are virulence factors enabling immune evasion and permanent colonization of the mammalian host, by mechanisms that are poorly understood. Recently, we demonstrated that free phosphocholine (PC) and PC-modified lipooligosaccharides (PC-LOS) from Haemophilus influenzae, an opportunistic pathogen of the upper and lower airways, function as unconventional nicotinic agonists and efficiently inhibit the ATP-induced release of monocytic IL-1β. We hypothesize that… Show more

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Cited by 13 publications
(17 citation statements)
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“…Whether stimulation of immune cells with nAChR agonists induces ion-channel functions is unclear. In most studies, no ion-currents have been detected in response to nAChR agonists (Peng et al, 2004; Razani-Boroujerdi et al, 2007; Hecker et al, 2009, 2015; Mikulski et al, 2010; Richter et al, 2016, 2018a; Zakrzewicz et al, 2017). However, stimulation of murine intestinal macrophages with agonists of α7 nAChR evoked small Ca 2+ transients (Matteoli et al, 2014).…”
Section: Introductionmentioning
confidence: 99%
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“…Whether stimulation of immune cells with nAChR agonists induces ion-channel functions is unclear. In most studies, no ion-currents have been detected in response to nAChR agonists (Peng et al, 2004; Razani-Boroujerdi et al, 2007; Hecker et al, 2009, 2015; Mikulski et al, 2010; Richter et al, 2016, 2018a; Zakrzewicz et al, 2017). However, stimulation of murine intestinal macrophages with agonists of α7 nAChR evoked small Ca 2+ transients (Matteoli et al, 2014).…”
Section: Introductionmentioning
confidence: 99%
“…Apart from conventional nAChR agonists, phosphocholine stimulates monocytic nAChRs and inhibits ATP-induced IL-1β release (Hecker et al, 2015; Richter et al, 2016, 2018a,b; Figure 1). The response of monocytic cells to free phosphocholine resembles that of choline: IC 50 values are in the range of 10 μM, signaling involves nAChR subunits α7, α9, and α10, both compounds do not elicit ion-currents at U937 cells, but inhibit the ion-channel function of the P2X7R (Hecker et al, 2015; Richter et al, 2016).…”
Section: Introductionmentioning
confidence: 99%
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“…Lastly, conotoxins are among the most rapidly evolving gene products known in nature and have served as tools in a diverse range of studies on the effects of feeding ecology, prey taxa, dietary breadth, age and geographical heterogeneity on the evolution of venom genes [72][73][74][75][76], and studies on the role of gene duplication and positive selection on venom gene expression and diversification [77][78][79]. Elucidating peptide biosynthesis and folding [68][69][70] α-ImI α7 nAChR Subtype selectivity [56] Targeted drug delivery in cancer [62], engineering D. melanogaster as better human disease model [61], chromaffin cell signaling [57] α-MII nAChR Subtype selective [80] Inflammation [81], reward and addiction [82,83] α-Vc1.1 and α-Rg1A α9α10 nAChR Subtype selective [84,85] Neuropathic pain and inflammation [86][87][88], immunology [89][90][91] Con-ikot-ikot AMPA receptor…”
Section: Research Toolsmentioning
confidence: 99%