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The inhibition of pepsin-catalysed reactions by structural and stereochemical product analogues

机译:结构和立体化学产物类似物抑制胃蛋白酶催化的反应

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p1. The inhibition of pepsin-catalysed hydrolysis of iN/i-acetyl-l-phenylalanyl-l-phenylalanylglycine by products and product analogues was studied. 2. Inhibitors of the l-configuration give rise to linear non-competitive inhibition, whereas those of the d-configuration show linear competitive behaviour. 3. Non-competitive inhibition by the product iN/i-acetyl-l-phenylalanine indicates an ordered release of products, which supports a common mechanism (involving an ‘amino-enzyme’) for pepsin-catalysed transpeptidation and hydrolysis reactions. 4. The differences in the types of inhibition caused by product analogues of the l- and d-series emphasize the stereospecificity of the binding of these inhibitors to free enzyme and to the putative amino-enzyme intermediate. 5. The results suggest that it is the anion of the acyl product that is released first in the hydrolytic reaction (see Kitson & Knowles, 1971)./p
机译:> 1。研究了胃蛋白酶催化产物和产物类似物对 N -乙酰基-1-苯丙氨酰基-1-苯丙氨酰基甘氨酸水解的抑制作用。 2.l-构型的抑制剂引起线性非竞争性抑制,而d-构型的抑制剂表现出线性竞争行为。 3.产物 N -乙酰基-1-苯丙氨酸的非竞争性抑制表明产物有序释放,这支持胃蛋白酶催化的转肽作用的共同机制(涉及“氨基酶”)。水解反应。 4.由l系列和d系列的产物类似物引起的抑制类型的差异强调了这些抑制剂与游离酶和推定的氨基酶中间体结合的立体特异性。 5.结果表明在水解反应中首先释放的是酰基产物的阴离子(参见Kitson& Knowles,1971)。

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