Odorant Inhibition of the Olfactory Cyclic Nucleotide-gated Channel with a Native Molecular Assembly

doi:10.1085/jgp.200609577

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Published online Aug 28 2006. doi:10.1085/jgp.200609577
The Rockefeller University Press, 0022-1295 $8.00
JGP, Volume 128, Number 3, 365-371

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ARTICLE

Odorant Inhibition of the Olfactory Cyclic Nucleotide-gated Channel with a Native Molecular Assembly

Tsung-Yu Chen¹, Hiroko Takeuchi², and Takashi Kurahashi²

¹ Center for Neuroscience and Department of Neurology, University of California, Davis, CA 95616
² Department of Frontier Biosciences, Osaka University, Toyonaka, Osaka 560-8531, Japan

Correspondence to Tsung-Yu Chen: tycchen{at}ucdavis.edu

Human olfaction comprises the opposing actions of excitationand inhibition triggered by odorant molecules. In olfactoryreceptor neurons, odorant molecules not only trigger a G-protein–coupledsignaling cascade but also generate various mechanisms to finetune the odorant-induced current, including a low-selectiveodorant inhibition of the olfactory signal. This wide-rangeolfactory inhibition has been suggested to be at the level ofion channels, but definitive evidence is not available. Here,we report that the cyclic nucleotide-gated (CNG) cation channel,which is a key element that converts odorant stimuli into electricalsignals, is inhibited by structurally unrelated odorants, consistentwith the expression of wide-range olfactory inhibition. Interestingly,the inhibitory effect was small in the homo-oligomeric CNG channelcomposed only of the principal channel subunit, CNGA2, but becamelarger in channels consisting of multiple types of subunits.However, even in the channel containing all native subunits,the potency of the suppression on the cloned CNG channel appearedto be smaller than that previously shown in native olfactoryneurons. Nonetheless, our results further showed that odorantsuppressions are small in native neurons if the subsequent molecularsteps mediated by Ca²⁺ are removed. Thus, the present work alsosuggests that CNG channels switch on and off the olfactory signalingpathway, and that the on and off signals may both be amplifiedby the subsequent olfactory signaling steps.

Abbreviations used in this paper: AA, amyl acetate; ANI, anisole;CIN, cineole; CNG, cyclic nucleotide-gated; IAA, isoamyl acetate;LIM, limonene.

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