Olfactory sensitivity to catecholamines and their metabolites in the goldfish. | - CCMAR -

Journal Article

TítuloOlfactory sensitivity to catecholamines and their metabolites in the goldfish.
Publication TypeJournal Article
AuthorsHubbard, PC, Barata, EN, Canario, AVM
Year of Publication2003
JournalChem Senses
Volume28
Questão3
Date Published2003 Mar
Pagination207-18
ISSN0379-864X
Palavras-chaveAction Potentials, Adrenergic alpha-Antagonists, Adrenergic beta-Antagonists, Animals, Catecholamines, Dopamine, Electrodes, Electrophysiology, Epinephrine, Female, Goldfish, Male, Norepinephrine, Olfactory Pathways, Receptors, Adrenergic, Smell, Stimulation, Chemical
Abstract

The current study assessed the olfactory sensitivity of the goldfish (Carassius auratus L.) to the catecholamines, their immediate precursors and metabolites by use of the electro-olfactogram (EOG). The olfactory system of the goldfish was found to be sensitive to both adrenaline and dopamine with thresholds of detection of 10(-7.8) and 10(-7.9) M respectively, but less so to noradrenaline (threshold of detection 10(-6.3) M). The 3-O-methoxy metabolites (metadrenaline, normetadrenaline and 3-O-methoxytyramine) evoked larger amplitude EOGs than the non-metabolized form with lower thresholds of detection. However, the olfactory system was less sensitive to the amino acid precursors L-tyrosine and L-DOPA, and markedly less so to the alpha-deaminated metabolites (3,4-dihydroxyphenyl glycol, 3,4-dihydroxy mandelic acid and dihydroxyphenyacetic acid). Sensitivity to metabolites, both alpha-deaminated and 3-O-methoxylated, was similar to the alpha-deaminated forms. Cross-adaptation studies suggested that, while there is some degree of commonality of the receptor mechanisms with L-tyrosine and L-serine, a proportion of the response to the catecholamines is due to distinct receptor subtypes. Similarly, the 3-O-methoxy metabolites also had (a) separate receptor mechanism(s), although, again, there was overlap with the adrenaline/dopamine receptor site(s). Presence of the alpha-adrenoreceptor antagonist prazosin or the peripheral DA(2) dopamine receptor antagonist domperidone caused partial attenuation of the EOG responses to adrenaline and dopamine, but had much less effect on the responses to their 3-O-methoxy metabolites. The beta-adrenoreceptor antagonist sotalol had no such effect. This suggests that the olfactory catecholamine receptors are structurally and functionally distinct from systemic adreno- and dopamine receptors. The current study raises the possibility that release of catecholamines or their 3-O-methoxy metabolites to the water may play a role in chemical communication.

Sapientia

http://www.ncbi.nlm.nih.gov/pubmed/12714443?dopt=Abstract

Alternate JournalChem. Senses
PubMed ID12714443
CCMAR Authors