
Biological and Pharmaceutical Bulletin p. 1361 - 1363 (1998)
Update date:2022-08-03
Topics:
Wu, Xiuzhong
Ono, Yoko
Noda, Atsuko
Noda, Hiroshi
The enantioselective N-acetylation of N-desisopropylpropranolol (NDP), one of the main metabolites of propranolol (PL), by rat liver acetyltransferase (AT), was investigated. R(+)-NDP or S(-)-NDP was used as a substrate at concentrations ranging from 10 to 200 μM. The cytosol fraction of a rat liver containing 3.93 mg protein/ml served as the source of AT. For 1-amino-3-(1-naphthyloxy)-2-propanol (AcNDP) formation from R(+)-NDP or s(- )-NDP in the presence of infinite AcCoA (250 μM), the K(m) value was calculated to be 67.5 or 62.4 μM, and the V(max) value was 0.462 or 0.205 nmol/min/mg protein. Based on these findings, the enantioselective N- acetylation of NDP was proved, i.e., AcNDP formation from R(+)-NDP was found to take place more easily than that from S(-)-NDP. Furthermore, AcNDP formation from NDP was competitively inhibited by the exogenous arylamine, p- aminobenzoic acid (PABA), which is well-known to be a typical substrate of AT. The presence of enantioselective inhibition for AcNDP formation was thus confirmed based on the K(i) values, 440 μM in the case of R(+)-NDP and 250 μM in the case of S(-)-NDP, respectively, i.e. two-fold enantioselective inhibition was demonstrated based on the Ki values in S(-)-enantiomer in comparison with R(+)-enantiomer.
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