Tyramine and Octopamine Independently Inhibit Serotonin-Stimulated Aversive Behaviors in Caenorhabditis elegans through Two Novel Amine Receptors

doi:10.1523/JNEUROSCI.3495-07.2007

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The Journal of Neuroscience, December 5, 2007, 27(49):13402-13412; doi:10.1523/JNEUROSCI.3495-07.2007

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Behavioral/Systems/Cognitive
Tyramine and Octopamine Independently Inhibit Serotonin-Stimulated Aversive Behaviors in Caenorhabditis elegans through Two Novel Amine Receptors
Rachel T. Wragg, Vera Hapiak, Sarah B. Miller, Gareth P. Harris, John Gray, Patricia R. Komuniecki, and Richard W. Komuniecki
Department of Biological Sciences, University of Toledo, Toledo, Ohio 43606-3340
Correspondence should be addressed to Richard W. Komuniecki, Department of Biological Sciences, University of Toledo, 2801 West Bancroft Street, Toledo, OH 43606-3340. Email: rkomuni{at}uoft02.utoledo.edu
Biogenic amines modulate key behaviors in both vertebrates andinvertebrates. In Caenorhabditis elegans, tyramine (TA) andoctopamine (OA) inhibit aversive responses to 100%, but notdilute (30%) octanol. TA and OA also abolish food- and serotonin-dependentincreases in responses to dilute octanol in wild-type but nottyra-3(ok325) and f14d12.6(ok371) null animals, respectively,suggesting that TA and OA modulated responses to dilute octanolare mediated by separate, previously uncharacterized, G-protein-coupledreceptors. TA and OA are high-affinity ligands for TYRA-3 andF14D12.6, respectively, based on their pharmacological characterizationafter heterologous expression. f14d12.6::gfp is expressed inthe ASHs, the neurons responsible for sensitivity to diluteoctanol, and the sra-6-dependent expression of F14D12.6 in theASHs is sufficient to rescue OA sensitivity in f14d12.6(ok371)null animals. In contrast, tyra-3::gfp appears not to be expressedin the ASHs, but instead in other neurons, including the dopaminergicCEP/ADEs. However, although dopamine (DA) also inhibits 5-HT-dependentresponses to dilute octanol, TA still inhibits in dop-2; dop-1;dop-3 animals that do not respond to DA and cat-2(tm346) andPdat-1::ICE animals that lack significant dopaminergic signaling,suggesting that DA is not an intermediate in TA inhibition.Finally, responses to TA and OA selectively desensitize afterpreexposure to the amines. Our data suggest that although tyraminergicand octopaminergic signaling yield identical phenotypes in theseolfactory assays, they act independently through distinct receptorsto modulate the ASH-mediated locomotory circuit and that C.elegans is a useful model to study the aminergic modulationof sensory-mediated locomotory behaviors.

Key words: olfaction; tyramine; adaptation; behavior; C. elegans; octopamine

Received Aug. 1, 2007; revised Oct. 16, 2007; accepted Oct. 16, 2007.

Correspondence should be addressed to Richard W. Komuniecki, Department of Biological Sciences, University of Toledo, 2801 West Bancroft Street, Toledo, OH 43606-3340. Email: rkomuni{at}uoft02.utoledo.edu