Studies on the metabolism of benoxinate by human pseudocholinesterase.

R Dubbels, W Schloot
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Abstract

The local anesthetic drug benoxinate (oxybuprocaine, Novesine) is hydrolyzed to 3-butoxy-4-aminobenzoic acid. A rapid and simple spectrophotometric method for benoxinate hydrolysis by human plasma was developed. Benoxinate is hydrolyzed enzymatically by an esterase present in the serum. Heat stability characteristics and apparent affinity values of the benoxinate metabolizing enzyme were in the same range compared to benzoylcholine chloride hydrolysis. Apparent Vmax-values differ by a mean factor of about 18 between the hydrolysis of both substrates. Considerable interindividual variability of benoxinate hydrolysis and inhibition of the enzymatic reaction by dibucaine and sodium fluoride has been observed. Furthermore, enzyme activity with benoxinate as substrate is positively correlated (P less than 0.001) with benzoylcholine chloride hydrolysis. Therefore, we assume that benoxinate is metabolized by human pseudocholinesterase (PCHE, E.C. 3.1.1.8) and that ocular side effects after benoxinate application may be caused by altered metabolism of this drug, depending on genetically determined variants of pseudocholinesterase.

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人假胆碱酯酶代谢苯氧酯的研究。
局部麻醉药物苯氧酸酯(羟布鲁卡因,诺维辛)水解成3-丁氧基-4-氨基苯甲酸。建立了一种快速、简便的分光光度法测定人血浆中苯甲酸酯水解的方法。苯氧苄酯被存在于血清中的酯酶水解。与苯甲酰氯胆碱水解酶相比,苯氧酯代谢酶的热稳定性和表观亲和值在相同的范围内。在两种底物的水解过程中,表观vmax值平均相差约18倍。已经观察到苯甲酸酯水解和二布卡因和氟化钠对酶促反应的抑制具有相当大的个体间差异。此外,以苯甲酰胆碱为底物的酶活性与苯甲酰胆碱水解呈正相关(P < 0.001)。因此,我们假设苯氧酸盐是由人假胆碱酯酶代谢的(PCHE, E.C. 3.1.1.8),苯氧酸盐应用后的眼部副作用可能是由药物代谢的改变引起的,这取决于基因决定的假胆碱酯酶的变异。
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