Koukiekolo R, Le Berre-Anton V, Desseaux V, Moreau Y, Rougé P, Marchis-Mouren G, Santimone M
Laboratoire de Biochimie et Biologie de la Nutrition CNRS ESA 6033, Faculté des Sciences et techniques de St Jérôme, Université d'Aix-Marseille, France.
Eur J Biochem. 1999 Oct 1;265(1):20-6. doi: 10.1046/j.1432-1327.1999.00611.x.
The effects of Phaseolus vulgaris inhibitor (alpha-AI) on the amylose and maltopentaose hydrolysis catalysed by porcine pancreatic alpha-amylase (PPA) were investigated. Based on a statistical analysis of the kinetic data and using the general velocity equation, which is valid at equilibrium for all types of inhibition in a single-substrate reaction, it was concluded that the inhibitory mode is of the mixed noncompetitive type involving two molecules of inhibitor. In line with this conclusion, the Lineweaver-Burk primary plots intersect in the second quadrant and the secondary plots of the slopes and the intercepts versus the inhibitor concentrations are parabolic curves, whether the substrate used was amylose or maltopentaose. A specific inhibition model of the mixed noncompetitive type applies here. This model differs from those previously proposed for acarbose [Al Kazaz, M., Desseaux, V., Marchis-Mouren, G., Payan, F., Forest, E. & Santimone, M. (1996) Eur. J. Biochem. 241, 787-796 and Al Kazaz, M., Desseaux, V., Marchis-Mouren, G., Prodanov, E. & Santimone, M. (1998) Eur. J. Biochem. 252, 100-107]. In particular, with alpha-AI, the inhibition takes place only when PPA and alpha-AI are preincubated together before the substrate is added. This shows that the inhibitory PPA-alphaAI complex is formed during the preincubation period. Secondly, other inhibitory complexes are formed, in which two molecules of inhibitor are bound to either the free enzyme or the enzyme-substrate complex. The catalytic efficiency was determined both with and without inhibitor. Using the same molar concentration of inhibitor, alpha-AI was found to be a much stronger inhibitor than acarbose. However, when the inhibitor amount is expressed on a weight basis (mg x L-1), the opposite conclusion is drawn. In addition, limited proteolysis was performed on PPA alone and on the alpha-AI-PPA complex. The results show that, in the complex, PPA is more sensitive to subtilisin attack, and shorter fragments are obtained. These data reflect the conformational changes undergone by PPA as the result of the protein inhibitor binding, which differ from those previously observed with acarbose.
研究了菜豆抑制剂(α - AI)对猪胰α -淀粉酶(PPA)催化直链淀粉和麦芽五糖水解的影响。基于动力学数据的统计分析并使用通用速度方程(该方程在单底物反应中对所有类型的抑制在平衡时均有效),得出抑制模式为涉及两分子抑制剂的混合型非竞争性抑制。与此结论一致,无论使用的底物是直链淀粉还是麦芽五糖,Lineweaver - Burk原始图在第二象限相交,斜率和截距相对于抑制剂浓度的次级图为抛物线。此处适用混合型非竞争性抑制的特定模型。该模型与先前针对阿卡波糖提出的模型不同[Al Kazaz, M., Desseaux, V., Marchis - Mouren, G., Payan, F., Forest, E. & Santimone, M. (1996) Eur. J. Biochem. 241, 787 - 796和Al Kazaz, M., Desseaux, V., Marchis - Mouren, G., Prodanov, E. & Santimone, M. (1998) Eur. J. Biochem. 252, 100 - 107]。特别是,对于α - AI,只有当PPA和α - AI在添加底物之前预先一起孵育时才会发生抑制。这表明抑制性PPA - αAI复合物在预孵育期间形成。其次,还形成了其他抑制性复合物,其中两分子抑制剂与游离酶或酶 - 底物复合物结合。测定了有无抑制剂时的催化效率。使用相同摩尔浓度的抑制剂时,发现α - AI比阿卡波糖是更强的抑制剂。然而,当以重量为基础表示抑制剂用量(mg×L⁻¹)时,得出相反的结论。此外,对单独的PPA和α - AI - PPA复合物进行了有限的蛋白酶解。结果表明,在复合物中,PPA对枯草杆菌蛋白酶的攻击更敏感,得到的片段更短。这些数据反映了由于蛋白质抑制剂结合而使PPA发生的构象变化,这与先前观察到的阿卡波糖的情况不同。
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