蜜蜂血淋巴α -糖苷酶特异性的表征和与酶不对称原体的底物定向聚集相关的明显协同性。

M Bounias
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引用次数: 0

摘要

基于实验确定的糖苷酶分子形态、特异性和对海藻糖(1.4)和蔗糖(0.6)的表观希尔系数,提出了一个涉及单个酶原聚体不同类型非随机聚集的理论模型。这个基本单元包含一个海藻糖特异性位点和两个不对称的亚位点:一个具有催化区,两者对任何底物非特异性结合区都具有适当的亲和力。然后,预测的启动子对二聚体、三聚体和四聚体的聚集可能性非常接近地解释了所有实验确定的酶的性质。此外,在培养基中高浓度海藻糖或蔗糖预孵育后观察到的酶多态性差异支持了酶聚集可能由培养基中主要浓度的特定底物指导的假设。
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Characterization of the honeybee haemolymph alpha-glycosidase specificity and apparent cooperativity as related to substrate-directed aggregation of enzyme asymmetric protomers.

Based on experimentally determined glycosidase molecular forms, their specificity and apparent Hill coefficients against trehalose (1.4) and sucrose (0.6), respectively, in honeybee haemolymph, a theoretical model is proposed involving differential types of non-random aggregation of a single enzyme protomer. This basic unit contains one trehalose-specific site and two asymmetrical subsites: one holds a catalytic zone and both share a proper affinity to any substrate non-specific binding zone. Then, the predicted aggregation possibilities of the promoter to dimers, trimers and tetramers very closely account for all the experimentally determined properties of the enzymes. Moreover, the hypothesis that the enzyme aggregation may be directed by the particular substrate present in major concentrations in the medium is supported by the observed differences in enzyme polymorphism following pre-incubation at high concentrations of either trehalose or sucrose in the medium.

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