The Cloned Capsaicin Receptor Integrates Multiple Pain-Producing Stimuli

Tominaga, Makoto; Caterina, Michael J.; Malmberg, Annika B.; Rosen, Tobias A.; Gilbert, Heather; Skinner, Kate; Raumann, Brigitte E; Basbaum, Allan I.; Julius, David

doi:10.1016/s0896-6273(00)80564-4

Cited by 2,811 publications

(2,496 citation statements)

References 51 publications

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“…The results presented here would suggest, therefore, that tissue acidosis is not itself a primary contributor to the pain observed in the CFA‐induced arthritis model, which might perhaps explain the lack of relief from either mechanical or thermal hyperalgesia in mice lacking ASIC1, ASIC2 or ASIC3 34. Although TRPV1 knockout mice display diminished thermal hyperalgesia in the CFA model,33 this is likely due to a shift in the thermal sensitivity of TRPV1 activation resulting from inflammatory mediators such as nerve growth factor dependent removal of phosphatidylinositol 4,5‐bisphosphate inhibition of TRPV1,57 rather than due to acid‐mediated modulation of the TRPV1 thermal activation threshold, which can also occur 58…”

Section: Discussionmentioning

confidence: 99%

Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate

Wright

Husson

et al. 2018

NMR in Biomedicine

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Arthritic conditions are a major source of chronic pain. Furthering our understanding of disease mechanisms creates the opportunity to develop more targeted therapeutics. In rheumatoid arthritis (RA), measurements of pH in human synovial fluid suggest that acidosis occurs, but that this is highly variable between individuals. Here we sought to determine if tissue acidosis occurs in a widely used rodent arthritis model: complete Freund's adjuvant (CFA)‐induced inflammation. CFA robustly evoked paw and ankle swelling, concomitant with worsening clinical scores over time. We used magnetic resonance spectroscopic imaging of hyperpolarized [1‐13C]pyruvate metabolism to demonstrate that CFA induces an increase in the lactate‐to‐pyruvate ratio. This increase is indicative of enhanced glycolysis and an increased lactate concentration, as has been observed in the synovial fluid from RA patients, and which was correlated with acidosis. We also measured the 13CO2/H13CO3 − ratio, in animals injected with hyperpolarized H13CO3 −, to estimate extracellular tissue pH and showed that despite the apparent increase in glycolytic activity in CFA‐induced inflammation there was no accompanying decrease in extracellular pH. The pH was 7.23 ± 0.06 in control paws and 7.32 ± 0.09 in inflamed paws. These results could explain why mice lacking acid‐sensing ion channel subunits 1, 2 and 3 do not display any changes in mechanical or thermal hyperalgesia in CFA‐induced inflammation.

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Section: Discussionmentioning

confidence: 99%

Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate

Wright

Husson

et al. 2018

NMR in Biomedicine

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“…Evidence indicates a range of G protein-coupled receptors that include those for bradykinin, prostanoids, opioids, 5-hydroxytryptamine (5-HT1 receptor), histamine (H3 receptor), neuropeptide Y, somatostatin, vasoactive intestinal polypeptide, purines and galanin. Among the channels the TRPV1 is the best known and it can be activated by noxious temperatures, low extracellular pH and a series of lipid derivatives [2,[38][39][40][41]. TRPV1 activity can be regulated by the stimulation of certain G protein coupled receptors (bradykinin and prostaglandins) or tyrosine kinase receptor (NGF) [42,43].…”

Section: Prejunctional Modulation Of Cgrp Releasementioning

confidence: 99%

CGRP and migraine: neurogenic inflammation revisited

Geppetti

Capone²,

Trevisani

et al. 2005

J Headache Pain

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The term 'neurogenic inflammation' refers to a series of proinflammatory responses produced by the stimulation of peripheral terminals of a subset of primary sensory neurons and the subsequent release of the neuropeptides, calcitonin gene-related peptide (CGRP) and the tachykinins, substance P (SP) and neurokinin A (NKA) [1]. The neurons that produce inflammation comprise a heterogeneous cell population with A-delta and C fibres, defined as polymodal nociceptors because they sense thermal, chemical and high-threshold mechanical stimuli. These neurons express on their plasma membrane a large panel of excitatory and inhibitory receptors and channels, and some of these signalling proteins have been successfully used as targets for analgesic or anti-inflammatory drugs. Among the channels expressed on peptidergic primary sensory neurons, transient receptor potential vanilloid-1 (TRPV1) [2], activated by the xenobiotic capsaicin, the pungent ingredient of plants of the genus Capsicum, is of paramount importance. Capsaicin produces burning pain by stimulating TRPV1 and by releasing sensory neuropeptides causes neurogenic inflammation. However, high concentrations/doses of capsaicin have the ability, after an initial excitatory phase, to desensitise the sensory nerve terminals, thus reducing the transmission of sensory/pain signals and abolishing neurogenic inflammation [3, 4]. This specific feature of capsaicin has greatly contributed to define the role of this subset of sensory nerves in pathophysiological models of human diseases and has been Pierangelo Geppetti Jay Guido Capone Marcello Trevisani Paola Nicoletti Giovanni Zagli Maria Rosalia Tola Abstract For more than a century neurogenic inflammation has been proposed to have a role in various human diseases. The present review will cover the conceptual steps of the itinerary that has led to the conclusion that neurogenic inflammation is important in migraine. Of particular relevance for the object of this article is the observation that tachykinindependent neurogenic inflammatory responses are evident in rodents, but much less pronounced or absent in other mammal species, including man, whereas neurogenic vasodilatation, most likely mediated by CGRP, occurs in most mammalian species and also in man. Recent evidence that a CGRP receptor antagonist was effective in the treatment of migraine attack supports the hypothesis that neurogenic vasodilatation is a major underlying mechanism of migraine.

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“…TRPV1 is also activated by acid [43][44][45], heat [24], arachidoynlethanolamide (AFA and anandamide) [46,47] In addition to exogenous stimuli, TRPV1 is sensitized by a number of endogenous inflammatory mediators. TRPV1 has several consensus phosphorylation sites where phosphorylation by protein kinases A, C and G (PKA,C and G) or tyrosine kinase might take place [49][50][51].…”

Section: Activation Of Trpv1 In the Lungmentioning

confidence: 99%

“…The airway C-fiber response to acid has both transient and sustained components. Electrophysiological and pharmacological studies show that the TRPV1-mediated response to acid is sustained, while most of the ASIC-type receptors mediate brief transient responses [45,67].…”

Section: Acid Sensingmentioning

confidence: 99%

Is TRPV1 a useful target in respiratory diseases?

Takemura

Quarcoo

Niimi

et al. 2008

Pulmonary Pharmacology & Therapeutics

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This review focuses on the transient receptor potential vanilloid 1 (TRPV1). TRPV1 is a non-selective cation channel predominantly expressed in the cell membranes of sensory afferent fibers, which are activated multi-modally. In the mammalian respiratory system, immunohistochemical and electrophysiological studies have revealed heterogeneous localizations of TRPV1 channels in the airways and their presence in pleural afferents. TRPV1 channels in afferents are not only involved with sensory inputs, but also release several neuropeptides upon stimulation. These processes trigger pathophysiological effects (e.g. reflex bronchoconstriction, hypersecretion, cough, etc.) that cause various symptoms of airway diseases.Recent studies have identified several endogenous and exogenous substances that can activate TRPV1 in the lung. Because of its key role in initiating inflammatory processes, TRPV1 receptor antagonists have been proposed as therapeutic candidates. Therefore, a critical update of recent therapeutic results is also given in this review.

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The Cloned Capsaicin Receptor Integrates Multiple Pain-Producing Stimuli

Cited by 2,811 publications

References 51 publications

Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate

Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate

CGRP and migraine: neurogenic inflammation revisited

Is TRPV1 a useful target in respiratory diseases?

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The Cloned Capsaicin Receptor Integrates Multiple Pain-Producing Stimuli

Cited by 2,811 publications

References 51 publications

Increased hyperpolarized [1‐13C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized 13C‐labelled bicarbonate

Increased hyperpolarized [1‐13C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized 13C‐labelled bicarbonate

CGRP and migraine: neurogenic inflammation revisited

Is TRPV1 a useful target in respiratory diseases?

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Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate

Increased hyperpolarized [1‐¹³C] lactate production in a model of joint inflammation is not accompanied by tissue acidosis as assessed using hyperpolarized ¹³C‐labelled bicarbonate