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Incubation of 1321N1 human astrocytoma cells with carbachol resulted in a rapid loss of binding of [3H]N-methylscopolamine ([3H]NMS) to muscarinic cholinergic receptors measured at 4 degrees C on intact cells; loss of muscarinic receptors in lysates from the same cells measured with [3H]quinuclidinyl benzilate [( 3H]QNB) at 37 degrees C occurred at a slower rate. Upon removal of agonist from the medium, the lost [3H]NMS binding sites measured on intact cells recovered with a t1/2 of approximately 20 min, but only to the level to which [3H]QNB binding sites had been lost; no recovery of "lost" [3H]QNB binding sites occurred over the same period. Based on these data and the arguments of Galper et al. (Galper, J. B., Dziekan, L. C., O'Hara, D. S., and Smith, T. W. (1982) J. Biol. Chem. 257, 10344-10356) regarding the relative hydrophilicity of [3H]NMS versus [3H]QNB, it is proposed that carbachol induces a rapid sequestration of muscarinic receptors that is followed by a loss of these receptors from the cell. These carbachol-induced changes are accompanied by a change in the membrane form of the muscarinic receptor. Although essentially all of the muscarinic receptors from control cells co-purified with the plasma membrane fraction on sucrose density gradients, 20-35% of the muscarinic receptors from cells treated for 30 min with 100 microM carbachol migrated to a much lower sucrose density. This conversion of muscarinic receptors to a "light vesicle" form occurred with a t1/2 approximately 10 min, and reversed with a t1/2 approximately 20 min. In contrast to previous results in this cell line regarding beta-adrenergic receptors (Harden, T. K., Cotton, C. U., Waldo, G. L., Lutton, J. K., and Perkins, J. P. (1980) Science 210, 441-443), agonist binding to muscarinic receptors in the light vesicle fraction obtained from carbachol-treated cells was still regulated by GTP. One interpretation of these data is that agonists induce an internalization of muscarinic receptors with the retention of their functional interaction with a guanine nucleotide regulatory protein.
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
October 1993,
The Journal of biological chemistry,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
April 1997,
Journal of neurochemistry,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
January 1983,
The Journal of pharmacology and experimental therapeutics,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
September 1981,
European journal of pharmacology,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
December 1983,
The Journal of pharmacology and experimental therapeutics,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
November 1992,
The Journal of biological chemistry,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
August 2000,
The EMBO journal,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
June 1991,
Biochemical pharmacology,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
February 1979,
Nature,
T K Harden, and
L A Petch, and
S F Traynelis, and
G L Waldo
July 1983,
Lancet (London, England),
