首页> 外文期刊>Journal of Analytical Toxicology >A gas chromatographic-mass spectrometric approach to examining stereoselective interaction of human plasma proteins with soman.
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A gas chromatographic-mass spectrometric approach to examining stereoselective interaction of human plasma proteins with soman.

机译:气相色谱-质谱法,用于检测人血浆蛋白与梭曼的立体选择性相互作用。

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摘要

The organophosphorus (OP) nerve agent soman (GD) contains two chiral centers (a carbon and a phosphorus atom), resulting in four stereoisomers (C+P+, C-P+, C+P-, and C-P-); the P- isomers exhibit a mammalian toxicity that is approximately 1000-fold greater than that of the P+ isomers. The capacity to assess the binding or hydrolysis of each of the four stereoisomers is an important tool in the development of enzymes with the potential to protect against GD intoxication. Using a gas chromatography-mass spectrometry-based approach, we have examined the capacity of plasma-derived human serum albumin, plasma-purified human butyrylcholinesterase, goat milk-derived recombinant human butyrylcholinesterase, and recombinant human paraoxonase 1 to interact with each of the four stereoisomers of GD in vitro at pH 7.4 and 25 degrees C. Under these experimental conditions, the butyrylcholinesterase samples were found to bind GD with a relative preference for the more toxic stereoisomers (C-P- > C+P- > C-P+ > C+P+),while human serum albumin and paraoxonase 1 interacted with GD with a relative preference for the less toxic isomers (C-P+/C+P+ > C+P-/C-P-). The results indicate that these human proteins exhibit distinct stereoselective interactions with GD. The approach described presents a means to rapidly assess substrate stereospecificity, supporting future efforts to develop more effective OP bioscavenger proteins.
机译:有机磷(OP)神经毒剂梭曼(GD)包含两个手性中心(一个碳原子和一个磷原子),产生四个立体异构体(C + P +,C-P +,C + P-和C-P-); P-异构体的哺乳动物毒性比P +异构体的毒性高约1000倍。评估四种立体异构体中每一种的结合或水解的能力是开发具有抗GD中毒潜力的酶的重要工具。使用基于气相色谱-质谱的方法,我们检查了血浆衍生的人血清白蛋白,血浆纯化的人丁酰胆碱酯酶,山羊奶来源的重组人丁酰胆碱酯酶和重组人对氧磷酶1与这四种相互作用的能力。 GD的体外立体异构体,在pH 7.4和25摄氏度的条件下。在这些实验条件下,发现丁酰胆碱酯酶样品结合GD,相对毒性更大的立体异构体相对偏爱(CP-> C + P-> C-P +> C + P +),而人血清白蛋白和对氧磷酶1与GD相互作用,相对偏爱毒性较小的异构体(C-P + / C + P +> C + P- / CP-)。结果表明,这些人蛋白与GD表现出不同的立体选择性相互作用。所描述的方法提供了一种快速评估底物立体特异性的方法,支持了开发更有效的OP生物清除剂蛋白的未来工作。

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