The effect of group selective reagentsN-ethylmaleimide and dithiothreitol on histamine H1-receptor binding sites in the vascular smooth muscle membranes
- 1 May 1984
- journal article
- Published by Springer Nature in Inflammation Research
- Vol. 14 (3-4) , 561-565
- https://doi.org/10.1007/bf01973872
Abstract
The chemical nature of the histamine H1-receptors of beef aortic membranes has been elucidated by introducing two group selective reagents in the [3H]-mepyramine binding studies: dithiothreitol (DTT), a protein-disulphide group reducing reagent, andN-ethylmaleimide (NEM), a proteinthiol group alkylating agent. In the binding experiments, NEM independently inhibits [3H]-mepyramine binding. The inhibition is time and concentration dependent. DTT on the other hand potentiates the binding of the radioligand to its receptor and changes the affinity of histamine in competing for [3H]-mepyramine binding site. In the DTT-pretreated membranes (100 μM), histamine shows a higher affinity for [3H]-mepyramine binding (K i 0.35 μM) than in the untreated membranes (K i 3.7 μM). Comparison of the pharmacological studies on the DTT-treated rabbit aortic strips and above binding studies, revealed a good correlation between the changes in the affinity of histamine for its receptor, when DTT was present. The results suggest an important role of the S-S and SH groups in the function of aortic histamine H1-receptor.Keywords
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