2014
DOI: 10.1016/s1873-9946(14)60095-7
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DOP070 The FFA2 antagonist GLPG0974: opportunity to treat neutrophil-driven inflammation

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“…We have shown that the GPR84 agonist ZQ16 induces a rise in [Ca 2+ ]i, is a weak secretagogue (triggered a low level of degranulation), a modest chemoattractant and a weak activator of NADPH oxidase‐derived ROS in naïve neutrophils (Sundqvist et al, 2018). All these neutrophil functions were abolished by the GPR84 selective antagonist GLPG1205 (Labéguère et al, 2020; Vanhoutte et al, 2015), confirming the involvement of GPR84 in neutrophil activation. Furthermore, when we examined the GPR84‐mediated ROS production induced by ZQ16 in more detail, we found that the level of ROS could be significantly enhanced by pre‐treatment of the cells with either the priming agent TNF‐α or the actin cytoskeleton disrupting agent latrunculin A (Sundqvist et al, 2018).…”
Section: Expression and Function Of Gpr84 In Neutrophilsmentioning
confidence: 79%
“…We have shown that the GPR84 agonist ZQ16 induces a rise in [Ca 2+ ]i, is a weak secretagogue (triggered a low level of degranulation), a modest chemoattractant and a weak activator of NADPH oxidase‐derived ROS in naïve neutrophils (Sundqvist et al, 2018). All these neutrophil functions were abolished by the GPR84 selective antagonist GLPG1205 (Labéguère et al, 2020; Vanhoutte et al, 2015), confirming the involvement of GPR84 in neutrophil activation. Furthermore, when we examined the GPR84‐mediated ROS production induced by ZQ16 in more detail, we found that the level of ROS could be significantly enhanced by pre‐treatment of the cells with either the priming agent TNF‐α or the actin cytoskeleton disrupting agent latrunculin A (Sundqvist et al, 2018).…”
Section: Expression and Function Of Gpr84 In Neutrophilsmentioning
confidence: 79%