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Molecular Pharmacology, Vol 2, 335-340, Copyright © 1966 by the American Society for Pharmacology and Experimental Therapeutics
1 Department of Pharmacology, University of Minnesota, Minneapolis, Minnesota 55455
SKF 525-A and its secondary and primary amine analogs, 2-ethylaminoethyl 2,2-diphenylvalerate HCl (SKF 8742-A) and 2-aminoethyl 2,2-diphenylvalerate HBr (AEDV), were compared for their effects on (a) the rate of hexobarbital metabolism in the intact rat, (b) hexobarbital sleeping time, and (c) rate of hexobarbital metabolism by the isolated perfused liver. The three compounds were found to be equipotent inhibitors by all three measurements. However, when the time interval between the injections of the inhibitor and the hexobarbital was increased from 45 min to 5 hr, SKF 525-A prolonged sleeping time longer than SKF 8742-A, and SKF 8742-A was more effective than AEDV. These results are interpreted to support the view that N-dealkylation plays an important role in the inhibition of drug metabolism by SKF 525-A.
Note:
ACKNOWLEDGMENT
This research was supported by USPHS grant
No. GM-12543. Part of this material appears in
abstract form in The Pharmacologist 7, 159 (1965).
The authors gratefully acknowledge the able
technical assistance of Mrs. Shirley Green.
This article has been cited by other articles:
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  T. R. Tephly, F. Tinelli, and W. D. Watkins Alcohol Metabolism: Role of Microsomal Oxidation in vivo Science, October 31, 1969; 166(3905): 627 - 628. [Abstract] [PDF]
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