Identification of novel target molecules of l-menthol

The present study used a binding assay to identify novel target biomolecules of l-menthol ([−]-menthol) that promote mouse ambulation. Among 88 different ligands to specific biomolecules examined, 0.1 mM l-menthol inhibited the binding of 13 ligands with relatively high inhibition rates. The assays showed that l-menthol acts on calcium channels, sodium channels, γ-aminobutyric acid type A (GABA(A)) receptor, GABA transporter, dopamine transporter, dopamine D4 receptor, adenosine A2a receptor, α2A-adrenergic receptor, histamine H2 receptor, bombesin receptor, angiotensin AT1 receptor, vasopressin V2 receptor, and leukotriene B4 receptor over a similar concentration range. The inhibition constant (K(i)) for l-menthol inhibition of binding of [(3)H]-WIN35,428 to the human recombinant dopamine transporter was 6.15 × 10(−4) mol/L. The K(i) for l-menthol inhibition of binding of [(3)H]-ethynylbicycloorthobenzoate (EBOB), a ligand of GABA(A) receptor picrotoxin site, was 2.88 × 10(−4) mol/L. These results should aid future research by providing clues for investigating the mechanisms underlying l-menthol activities, including the ambulation-promoting effect. The present results suggest that the dopamine transporter, adenosine A2a receptor, dopamine D4 receptor, α2A-adrenergic receptor, and GABA(A) receptor are promising candidate molecules that are involved in the mechanisms underlying the psychostimulant-like effect of l-menthol.