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首页> 外文期刊>Archives of Toxicology >An in vitro approach for demonstrating the critical role of serum albumin in the detoxication of the carbamate carbaryl at in vivo toxicologically relevant concentrations.
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An in vitro approach for demonstrating the critical role of serum albumin in the detoxication of the carbamate carbaryl at in vivo toxicologically relevant concentrations.

机译:在体内毒理学相关浓度下证明血清白蛋白在氨基甲酸酯西维因脱毒中的关键作用的体外方法。

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The hydrolysis of carbaryl by bovine serum albumin (BSA) was studied at toxicologically relevant concentrations (range 15-300 muM) in order to determine the role of this protein in the detoxication of the carbamate in vivo. The 1-naphthol released during the hydrolysis of carbaryl was monitored using gas chromatography coupled with mass spectrometry. BSA hydrolyzed carbaryl in a time-progressive way. The hydrolysis was also dependent of enzyme (1.0, 2.5, 5.0 and 7.0 mg ml(-1)) and substrate (range between 15 and 1,000 muM) concentration. The estimated turnover number and Michaelis-Menten constant were 1.6 x 10(-4) s(-1) and 430 muM, respectively. Thus, the second order rate constant was 0.37 M(-1) s(-1). At enzyme concentrations of 7.0 mg ml(-1) and substrate concentrations ranging between 50 and 300 muM about 80% of substrate was hydrolyzed in 3 h. At lower substrate concentrations (15 and 30 muM carbaryl) also significant hydrolysis was detected at the highest enzyme concentration, even when these substrate concentrations were 30 and 15 times lower than the Michaelis-Menten constant. Although the efficacy of the enzymatic hydrolysis is low, the extrapolation of our results to the physiological albumin high concentrations (around 40 mg ml(-1)) suggests that the hydrolysis of carbaryl by serum albumins plays a critical role in the detoxication of this carbamate at in vivo toxicologically relevant concentrations.
机译:为了确定该蛋白在体内氨基甲酸酯脱毒中的作用,在毒理学相关浓度(范围为15-300μM)下研究了牛血清白蛋白(BSA)对西维因的水解作用。使用气相色谱-质谱联用技术监测西维因水解过程中释放的1-萘酚。 BSA以时间递增的方式水解了西维因。水解还取决于酶(1.0、2.5、5.0和7.0 mg ml(-1))和底物(介于15和1,000μM之间)的浓度。估计的周转数和Michaelis-Menten常数分别为1.6 x 10(-4)s(-1)和430μM。因此,二阶速率常数为0.37 M(-1)s(-1)。在7.0 mg ml(-1)的酶浓度和50至300μM的底物浓度下,约80%的底物在3小时内被水解。在较低的底物浓度(15和30μM甲萘威)下,即使在这些底物浓度比Michaelis-Menten常数低30和15倍时,在最高酶浓度下也能检测到明显的水解。尽管酶水解的功效很低,但我们的结果推断到高浓度的生理白蛋白(约40 mg ml(-1))表明,血清白蛋白水解西维因在该氨基甲酸酯的解毒中起关键作用在体内毒理学相关浓度。

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