Menthol attenuates respiratory irritation responses to multiple cigarette smoke irritants

Willis, Daniel N.; Liu, Boyi; Ha, Michael A.; Jordt, Sven‐Eric; Morris, John B.

doi:10.1096/fj.11-188383

Cited by 160 publications

(146 citation statements)

References 60 publications

(99 reference statements)

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“…21,22 Evidence from the studies in mice also indicate that menthol's inhibitory effects depend upon TRPM8, which has been shown to underlie the analgesic effects of cold on acute and inflammatory pain via an opioid-dependent central neural pathway. 49 An analgesic action of menthol via a central neural mechanism raises the possibility that menthol stimulation in both the upper and lower airways may contribute to reducing the sensory irritation of nicotine that is sensed most acutely in the throat and lungs.…”

Section: Discussionmentioning

confidence: 99%

“…The authors of a recent study of menthol cigarettes concluded there was no consistent effect of menthol on perceived harshness and overall impact, 20 whereas a previous study indicated that menthol could either increase or decrease the perceived harshness of a cigarette depending on nicotine concentration. 8 Studies in mice 21,22 indicate that menthol can reduce the sensory irritation from constituents of cigarette smoke, including nicotine, that stimulate the pain receptor TRPA1, 23,24 which has been shown to play a role in cough. 25 However, the numerous other chemical and particulate irritants in tobacco smoke 5,26 have precluded direct measurement of the effect of menthol on the perception of nicotine irritation alone.…”

Section: Introductionmentioning

confidence: 99%

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Sensory Effects of Menthol and Nicotine in an E-Cigarette

Rosbrook

Green

2016

NICTOB

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Introduction: Despite the longstanding use and popularity of menthol as a flavorant in tobacco products, its sensory interactions with inhaled nicotine have never been measured independently of the other irritants in tobacco smoke. We therefore measured the perception of menthol in an E-cigarette with the primary goal of assessing its analgesic effect on the sensory irritation produced by inhaled nicotine. Methods: Adult cigarette smokers sampled aerosolized E-liquids containing five different concentrations of nicotine with 0%, 0.5%, or 3.5% l-menthol, as well as two commercial menthol flavors with and without nicotine. For each of the E-liquids participants used a labeled magnitude scale to rate the Overall Sensation intensity, Coolness/Cold, and Irritation/Harshness they experienced, and a Labeled Hedonic Scale to indicate how much they liked/disliked the overall flavor. Results: The main findings were that (1) perceived Irritation/Harshness was unaffected by a low (0.5%) menthol concentration, whereas a high menthol concentration (3.5%) led to higher perceived Irritation/Harshness at low nicotine concentrations but to lower Irritation/Harshness at the highest nicotine concentration (24 mg/ml); (2) a commercial Menthol-Mint flavor produced similar results; (3) nicotine tended to enhance rather than suppress sensations of Coolness/Cold; and (4) menthol tended to slightly increase liking independently of nicotine concentration. Conclusion: In addition to adding a sensation of coolness, menthol can reduce perceived airway irritation and harshness produced by inhalation when nicotine concentration is high, and contributes to the sensory impact of E-liquids when nicotine concentration is low. Implications: The evidence presented here indicates that menthol can potentially improve the appeal of E-cigarettes not only via its coolness and minty flavor, but also by reducing the harshness from high concentrations of nicotine. As the first direct demonstration of an analgesic effect of menthol on inhaled nicotine in humans, these data also have implications for the role of menthol flavors in other inhaled tobacco products.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Sensory Effects of Menthol and Nicotine in an E-Cigarette

Rosbrook

Green

2016

NICTOB

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“…The consequences of this effect are not known with certainty, but one possibility is that it could offset the irritant effects of nicotine in the airways, allowing cigarette smoke to be inhaled deeper into the lungs and held there for a longer time. Thus, the known analgesic effects of menthol, acting via sensory nerve TRPM8 (Willis et al, 2011) and TRPA1 channels, may be augmented by enhanced desensitization of sensory nerve nAChRs.…”

Section: Discussionmentioning

confidence: 99%

“…Menthol may be added to tobacco to deliver a distinct oral sensation, as it imparts a characteristic cooling sensation via activation of transient receptor potential channel, subfamily M, member 8 (TRPM8) ion channels expressed in a population of thermosensory nerves (McKemy et al, 2002;Peier et al, 2002;Bautista et al, 2007). In turn, signaling downstream of TRPM8 can lead to analgesia through undefined mechanisms (Willis et al, 2011). In addition, menthol may produce analgesic/counterirritant effects through activation and desensitization of the nociceptive transient receptor potential channel, subfamily A, member 1 (TRPA1) channel (Macpherson et al, 2006;Karashima et al, 2007;Xiao et al, 2008) or by direct antagonism of the TRPA1 channel (Karashima et al, 2007;Xiao et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Menthol Enhances the Desensitization of Human α3β4 Nicotinic Acetylcholine Receptors

et al. 2015

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The a3b4 nicotinic acetylcholine receptor (nAChR) subtype is widely expressed in the peripheral and central nervous systems, including in airway sensory nerves. The nAChR subtype transduces the irritant effects of nicotine in tobacco smoke and, in certain brain areas, may be involved in nicotine addiction and/or withdrawal. Menthol, a widely used additive in cigarettes, is a potential analgesic and/or counterirritant at sensory nerves and may also influence nicotine's actions in the brain. We examined menthol's effects on recombinant human a3b4 nAChRs and native nAChRs in mouse sensory neurons. Menthol markedly decreased nAChR activity as assessed by Ca 21 imaging, 86 Rb 1 efflux, and voltage-clamp measurements. Coapplication of menthol with acetylcholine or nicotine increased desensitization, demonstrated by an increase in the rate and magnitude of the current decay and a reduction of the current integral. These effects increased with agonist concentration. Pretreatment with menthol followed by its washout did not affect agonist-induced desensitization, suggesting that menthol must be present during the application of agonist to augment desensitization. Notably, menthol acted in a voltageindependent manner and reduced the mean open time of single channels without affecting their conductance, arguing against a simple channel-blocking effect. Further, menthol slowed or prevented the recovery of nAChRs from desensitization, indicating that it probably stabilizes a desensitized state. Moreover, menthol at concentrations up to 1 mM did not compete for the orthosteric nAChR binding site labeled by [ 3 H]epibatidine. Taken together, these data indicate that menthol promotes desensitization of a3b4 nAChRs by an allosteric action.

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“…In mice, irritancy induced by a wide range of protussive substances was inhibited by menthol, an effect that was antagonized by the TRPM8 antagonist AMTB (Willis et al, 2011). Recent evidence indicates that the antitussive activity of menthol may reside in the activation of nasal, as opposed to pulmonary sensory afferents (Plevkova et al, 2013), inferring that menthol inhibits cough by a central "gating" mechanism rather than any local antitussive activity.…”

Section: A Menthol and Trpm8 Agonistsmentioning

confidence: 99%