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Interactions of Paraoxonase-1 with Pharmacologically Relevant Carbamates

机译:具有药理学相关的氨基甲酸酯的律酶酶-1的相互作用

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Mammalian paraoxonase-1 hydrolyses a very broad spectrum of esters such as certain drugs and xenobiotics. The aim of this study was to determine whether carbamates influence the activity of recombinant PON1 (rePON1). Carbamates were selected having a variety of applications: bambuterol and physostigmine are drugs, carbofuran is used as a pesticide, while Ro 02-0683 is diagnostic reagent. All the selected carbamates reduced the arylesterase activity of rePON1 towards the substrate S-phenyl thioacetate (PTA). Inhibition dissociation constants (Ki), evaluated by both discontinuous and continuous inhibition measurements (progress curves), were similar and in the mM range. The rePON1 displayed almost the same values of Ki constants for Ro 02-0683 and physostigmine while, for carbofuran and bambuterol, the values were approximately ten times lower and two times higher, respectively. The affinity of rePON1 towards the tested carbamates was about 3–40 times lower than that of PTA. Molecular modelling of rePON1-carbamate complexes suggested non-covalent interactions with residues of the rePON1 active site that could lead to competitive inhibition of its arylesterase activity. In conclusion, carbamates can reduce the level of PON1 activity, which should be kept in mind, especially in medical conditions characterized by reduced PON1 levels.
机译:哺乳动物定律酶-1水解了一种非常广泛的酯,例如某些药物和异种术。本研究的目的是确定氨基甲酸酯是否会影响重组PON1(REPOR1)的活性。选择具有多种应用的氨基甲酸酯:Bambuterol和粪岛是药物,碳呋喃用作农药,而RO 02-0683是诊断试剂。所有选定的氨基甲酸酯将REPON1的芳基酯酶活性降低朝向底物S-苯基乙酸酯(PTA)。通过不连续和连续抑制测量(进展曲线)评估的抑制解离常数(KI)在MM范围内评估。 REPON1显示RO 02-0683和粪菌的ki常数值几乎相同,而对于碳呋喃和bambuterol,该值分别为约10倍,两倍倍增。 Repon1对测试氨基甲酸酯的亲和力比PTA低约3-40倍。 Repon1-carbamate复合物的分子建模建议与饲料1活性位点的残留物的非共价相互作用,这可能导致其芳基酯酶活性的竞争性抑制。总之,氨基甲酸酯可以减少PON1活性的水平,应该牢记,尤其是在病症的特征在于减少PON1水平。

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