Kinetic Investigations of Liver Microsomal Esterases with Oxazepam Esters
- 1 January 1978
- journal article
- research article
- Published by Walter de Gruyter GmbH in Hoppe-Seyler´s Zeitschrift Für Physiologische Chemie
- Vol. 359 (2), 879-886
- https://doi.org/10.1515/bchm2.1978.359.2.879
Abstract
Hepatic microsomal esterases of the mouse responsible for the bioactivation of inactive (prodrug) esters of the centrally acting oxazepam were studied. The enzymes are situated on the cytoplasmic side of the microsomes. The esterases are partly solubilized and partly inactivated by homogenization in aqueous glycerol and treatment with deoxycholate. There is good correlation between the rates of hydrolysis and steric constants of the acyl moiety. Substrate binding increases to an optimum with the number of carbon atoms in the acyl moiety and is of a hydrophobic nature. The esterases were classified on the basis of the effect of inhibitors and activators.This publication has 5 references indexed in Scilit:
- The Primary Specificity of Chymotrypsin. Further Evidence for “Wrong-Way” Binding*Biochemistry, 1966
- The reaction of organophosphorus compounds with hydrolytic enzymeS—II.Biochemical Pharmacology, 1966
- FRACTIONATION OF MOUSE LIVER MICROSOMAL ESTERASESCanadian Journal of Biochemistry, 1964
- Curtain Electrophoretic Separation of Phenyl Acetate Hydrolysing Esterases of Human Serum. Demonstration of an EDTA-Dependent Enzyme.Experimental Biology and Medicine, 1962
- The determination of enzyme inhibitor constantsBiochemical Journal, 1953