乙酰胆碱酯酶。有机磷化合物的两种抑制类型:一种是形成磷酸化酶,另一种类似于底物抑制。
Acetylcholinesterase. Two types of inhibition by an organophosphorus compound: one the formation of phosphorylated enzyme and the other analogous to inhibition by substrate.
作者信息
Aldridge W N, Reiner E
出版信息
Biochem J. 1969 Nov;115(2):147-62. doi: 10.1042/bj1150147.
Abstract
- The kinetics of the reaction of di-(2-chloroethyl) 3-chloro-4-methylcoumarin-7-yl phosphate (haloxon) and related compounds with acetylcholinesterase were studied and found to be unusual. 2. By a progressive reaction haloxon produces a di-(2-chloroethyl)phosphorylated enzyme. The influence of substrate on this reaction leading to a phosphorylated active centre was studied. From competition experiments between inhibitor and substrate values of K(m) for acetylcholine and acetylthiocholine of 0.79mm and 0.23mm respectively were derived. 3. Haloxon also combines with acetylcholinesterase by a non-progressive reaction, producing a complex that is reversible by dilution and by high concentrations of acetylcholine and acetylthiocholine. From this non-progressive reaction the competition between haloxon and substrate was studied, and it was shown that haloxon combines with a site involved in inhibition by substrate. From competition experiments the following dissociation constants were derived: for combination of haloxon and this site K(i) is 4.9mum and for the combination of substrates with this site K(88) values are 12mm and 3.3mm for acetylcholine and acetylthiocholine respectively. 4. The non-phosphorus-containing compound 3-chloro-7-hydroxy-4-methylcoumarin was shown to be a good reagent for the site involved in inhibition by substrate; its dissociation constant for the combination with this site is 30mum. 5. In order to interpret the experimental results, theoretical equations were derived for an enzyme with two binding sites to both of which substrate and inhibitor can combine. The equations correlate the activity of the enzyme with the concentration of substrate and inhibitor, for both progressive and non-progressive inhibition. These equations are applicable to reactions of acetylcholinesterase with organophosphorus compounds, carbamates etc. and may be applicable to other enzymes possessing two binding sites.
摘要
- 研究了二(2-氯乙基)3-氯-4-甲基香豆素-7-基磷酸酯(血防-67)及相关化合物与乙酰胆碱酯酶反应的动力学,发现其反应异常。2. 通过逐步反应,血防-67产生二(2-氯乙基)磷酸化酶。研究了底物对导致磷酸化活性中心的该反应的影响。从抑制剂与底物的竞争实验中,得出乙酰胆碱和乙酰硫代胆碱的米氏常数(K(m))值分别为0.79mmol/L和0.23mmol/L。3. 血防-67还通过非逐步反应与乙酰胆碱酯酶结合,形成一种复合物,该复合物可通过稀释以及高浓度的乙酰胆碱和乙酰硫代胆碱使其逆转。通过这种非逐步反应研究了血防-67与底物之间的竞争,结果表明血防-67与底物抑制所涉及的位点结合。从竞争实验中得出以下解离常数:血防-67与该位点结合的K(i)为4.9μmol/L,底物与该位点结合的K(88)值,乙酰胆碱和乙酰硫代胆碱分别为12mmol/L和3.3mmol/L。4. 不含磷的化合物3-氯-7-羟基-4-甲基香豆素被证明是底物抑制所涉及位点的良好试剂;其与该位点结合的解离常数为30μmol/L。5. 为了解释实验结果,推导了针对具有两个结合位点的酶的理论方程,底物和抑制剂均可与这两个位点结合。这些方程将酶的活性与底物和抑制剂的浓度相关联,适用于逐步抑制和非逐步抑制。这些方程适用于乙酰胆碱酯酶与有机磷化合物、氨基甲酸酯等的反应,也可能适用于具有两个结合位点的其他酶。
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