Functional expression of human D3 dopamine receptors in differentiated neuroblastoma × glioma NG108–15 cells

Abstract

This study describes the depression of calcium currents caused by activation of human D₃ dopamine receptors which have been stably expressed in the neuroblastoma × glioma NG108–15 cell line. Transfected cells, which had been differentiated with prostaglandin E₁ and isobutylmethylxanthine, exclusively expressed D₃ receptor mRNA, which was demonstrated by reverse transcription polymerase chain reaction techniques. Transfected cells had high affinity binding sites for iodosulpiride, with a K_d of 0.8 nm and receptor density of 240 fmolmg⁻¹ protein. Calcium currents were recorded using nystatinperforated patch clamp techniques. In contrast to untransfected cells that had been differentiated, high-threshold calcium currents in differentiated hD₃-NG108–15 cells were depressed by application of dopamine and quinpirole. These responses were abolished by the dopamine receptor antagonist S-(–)-sulpiride (1 μm), demonstrating that they were caused by the activation of the transfected dopamine receptors. Coupling of human D₃ receptors to calcium currents was sensitive to the action of pertussis toxin, suggesting the involvement of G-proteins of the G_i and/or G_o subtype. These results demonstrate that human D₃ receptors represent a functional class of dopamine receptor.