2002
DOI: 10.1073/pnas.152002699
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Bradykinin-12-lipoxygenase-VR1 signaling pathway for inflammatory hyperalgesia

Abstract: The capsaicin-sensitive vanilloid receptor (VR1) was recently shown to play an important role in inflammatory pain (hyperalgesia), but the underlying mechanism is unknown. We hypothesized that pain-producing inflammatory mediators activate capsaicin receptors by inducing the production of fatty acid agonists of VR1. This study demonstrates that bradykinin, acting at B2 bradykinin receptors, excites sensory nerve endings by activating capsaicin receptors via production of 12-lipoxygenase metabolites of arachido… Show more

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Cited by 339 publications
(305 citation statements)
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References 32 publications
(35 reference statements)
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“…So far, direct TRPV1 activation has been proposed for muscarinic-3 receptors (18) and metabotropic glutamate-5 receptors (55) via DAG production and for the B2R via PIP 2 degradation (17) or LOX activation (45). Herein, we noted that TRPV1 co-expression in F11-MRGPR-X1 cells profoundly enhanced MRGPR-X1-induced Ca 2ϩ signals, Mn 2ϩ influx, and cation currents at RT and constant pH, indicative of direct TRPV1 activation.…”
Section: Discussionmentioning
confidence: 99%
“…So far, direct TRPV1 activation has been proposed for muscarinic-3 receptors (18) and metabotropic glutamate-5 receptors (55) via DAG production and for the B2R via PIP 2 degradation (17) or LOX activation (45). Herein, we noted that TRPV1 co-expression in F11-MRGPR-X1 cells profoundly enhanced MRGPR-X1-induced Ca 2ϩ signals, Mn 2ϩ influx, and cation currents at RT and constant pH, indicative of direct TRPV1 activation.…”
Section: Discussionmentioning
confidence: 99%
“…That TRPV1 is important in pathological states is further suggested by its ability to respond, and be potentiated by, multiple stimuli including those that are physical (heat and mechanical) and chemical (e.g., vanilloid compounds and acid). In addition, TRPV1 currents can be potentiated by interactions with G-coupled proteins like the bradykinin receptors (Shin et al, 2002;Sugiura et al, 2002;Carr et al, 2003;Ferreira et al, 2004) and the P2Y2 ATP receptor (Moriyama et al, 2003). It is also important to note that behavioral heat hyperalgesia induced by either complete Freund's adjuvant, carrageenan, or ATP is absent in TRPV1 Ϫ/Ϫ mice (although pretreatment responses are normal) (Caterina et al, 2000;Davis et al, 2000;Moriyama et al, 2003).…”
Section: Discussionmentioning
confidence: 99%
“…These involve heat ( 43°C), acidosis (pH<5.9) [173] and mostly arachidonic acid derived lipid mediators such as the endocannabinoid anandamide [179,180], the "endovanilloid" N-arachidonoyl-dopamine [181], and lypoxigenase products [182,183]. Besides direct activation mechanisms, several molecules are able to act on TRPV1 via first activating their specific receptors and then initiating downstream signaling pathways leading to the sensitization of TRPV1.…”
Section: Activation and Sensitization Of Trpv1mentioning
confidence: 99%
“…Indeed, bradykinin [183,184], ATP [185], lipoxygenase products [182,183], prostaglandins [186,187], histamine [188], various neurotrophins (NGF, neurotrophin-3 and -4) [91,102,184], TNF- [189,190], pro-inflammatory chemokines [191], and PAR2 [192,193] were all reported to sensitize TRPV1 via various signal transduction pathways. TRPV1 was shown to be modulated by the protein kinase C (PKC) [183,[194][195][196], phospholipase C (PLC), and phosphatidylinositol 4,5-bisphosphate (PIP 2 ) [184,[197][198][199][200] systems as well as by intracellular ATP [201]. The sensitization process eventually results in the shift of the activation temperature and voltage threshold towards more physiological ranges [195,[202][203][204].…”
Section: Activation and Sensitization Of Trpv1mentioning
confidence: 99%