DESENSITIZATION OF PROSTACYCLIN RECEPTORS IN A NEURONAL HYBRID CELL LINE
Open Access
- 1 September 1982
- journal article
- research article
- Published by Wiley in British Journal of Pharmacology
- Vol. 77 (1) , 121-127
- https://doi.org/10.1111/j.1476-5381.1982.tb09277.x
Abstract
1 Prostacyclin and its stable analogue, carbacyclin, bind competitively to a single population of receptors, and activate adenylate cyclase of the NCB-20 neuronal somatic cell hybrid (Kact = 40.1 nM and 96.1 nM respectively). 2 Culture of NCB-20 cells in the presence of 1 μm carbacyclin for 4 to 16 h results in a progressive decrease in the prostacyclin-dependent activation of adenylate cyclase in cell homogenates with an increase at 16 h of the Kact from 64.1 nm to 174.0 nm and decrease in the maximum adenylate cyclase activation from 41.2 to 15.1 pmol cyclic AMP min−1 mg−1 protein. 3 The prediction that the apparent decrease in affinity in the prostacyclin-dependent activation of adenylate cyclase was secondary to a reduction in receptor numbers was tested directly by measuring binding of [3H]-prostacyclin to membranes of cells exposed to carbacyclin for 16 h. This showed an actual decrease in affinity of the prostacyclin-receptor interaction, as well as a decrease in the total receptor numbers. Thus prolonged exposure of NCB-20 cells to carbacyclin caused reductions in both receptor numbers and affinity, reflected by measurements both of binding and adenylate cyclase activation.This publication has 31 references indexed in Scilit:
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