Importance of the C-terminus of the human 5-HT3A receptor subunit

Amongst the family members of Cys-loop LGICs, the atypical ability of the 5-HT3A subunit to form functional homomeric receptors allowed a direct investigation of the role of the C-terminus. Deletion of the three C-terminal amino acids (Delta GIn(453)-Delta Tyr(454)-Delta Ala(455)) from the h5-HT3A subunit prevented formation of a specific radioligand binding site as well as expression within the cell membrane. Removal of merely the C-terminal residue (Delta Ala(455)) reduced specific radioligand binding(to 4 +/- 1% relative to the wild-type; cells grown at 37 degrees C and also cell membrane expression; these reductions were less evident when the Delta Ala(455) expressing cells were grown at 27 degrees C (specific radioligand binding levels 27 +/- 5% relative to wild-type also grown at 27 degrees C). Mutation of the h5-HT3A C-terminal amino acid, alanine, for either glycine (Ala(455)Gly), valine (Ala(455)Val) or leucine (Ala(455)Leu) reduced specific radioligand binding levels by 24 +/- 23%, 32 +/- 12% and 88 +/- 1%, respectively; the latter mutant also displaying reduced membrane expression. In contrast, mutation to alanine of the two amino acids preceding the C-terminal alanine (Gln(453) Ala and Tyr(454)Ala) had no detrimental effects on specific radioligand binding or cell membrane expression levels. The present study demonstrates an important role for the C-terminus in the formation of the functional h5-HT(3)A receptor. The partial restoration of 5-HT3 receptor binding and cell membrane expression when cells expressing C-terminal mutant 5-HT3A subunits were grown at a lower temperature (27 degrees C) suggests that the C-terminus stabilises the 5-HT3 receptor allowing subunit folding and subsequent maturation. (C) 2008 Published by Elsevier Ltd.