首页> 美国卫生研究院文献>Journal of Analytical Toxicology >Cyanide Toxicokinetics: The Behavior of Cyanide Thiocyanate and 2-Amino-2-Thiazoline-4-Carboxylic Acid in Multiple Animal Models
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Cyanide Toxicokinetics: The Behavior of Cyanide Thiocyanate and 2-Amino-2-Thiazoline-4-Carboxylic Acid in Multiple Animal Models

机译:氰化物的毒物动力学:多种动物模型中氰化物硫氰酸盐和2-氨基-2-噻唑啉-4-羧酸的行为

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摘要

Cyanide causes toxic effects by inhibiting cytochrome c oxidase, resulting in cellular hypoxia and cytotoxic anoxia, and can eventually lead to death. Cyanide exposure can be verified by direct analysis of cyanide concentrations or analyzing its metabolites, including thiocyanate (SCN) and 2-amino-2-thiazoline-4-carboxylic acid (ATCA) in blood. To determine the behavior of these markers following cyanide exposure, a toxicokinetics study was performed in three animal models: (i) rats (250–300 g), (ii) rabbits (3.5–4.2 kg) and (iii) swine (47–54 kg). Cyanide reached a maximum in blood and declined rapidly in each animal model as it was absorbed, distributed, metabolized and eliminated. Thiocyanate concentrations rose more slowly as cyanide was enzymatically converted to SCN. Concentrations of ATCA did not rise significantly above the baseline in the rat model, but rose quickly in rabbits (up to a 40-fold increase) and swine (up to a 3-fold increase) and then fell rapidly, generally following the relative behavior of cyanide. Rats were administered cyanide subcutaneously and the apparent half-life (t1/2) was determined to be 1,510 min. Rabbits were administered cyanide intravenously and the t1/2 was determined to be 177 min. Swine were administered cyanide intravenously and the t1/2 was determined to be 26.9 min. The SCN t1/2 in rats was 3,010 min, but was not calculated in rabbits and swine because SCN concentrations did not reach a maximum. The t1/2 of ATCA was 40.7 and 13.9 min in rabbits and swine, respectively, while it could not be determined in rats with confidence. The current study suggests that cyanide exposure may be verified shortly after exposure by determining significantly elevated cyanide and SCN in each animal model and ATCA may be used when the ATCA detoxification pathway is significant.
机译:氰化物通过抑制细胞色素C氧化酶而引起毒性作用,导致细胞缺氧和细胞毒性缺氧,最终可能导致死亡。可以通过直接分析血液中的氰化物浓度或分析其代谢产物(包括硫氰酸盐(SCN -)和2-氨基-2-噻唑啉-4-羧酸(ATCA))来验证氰化物的暴露。为了确定氰化物暴露后这些标志物的行为,对三种动物模型进行了毒物动力学研究:(i)大鼠(250–300 g),(ii)兔子(3.5–4.2 kg)和(iii)猪(47– 54公斤)。在每种动物模型中,氰化物的血液含量达到最大值,并被吸收,分配,代谢和消除,因此迅速下降。由于氰化物被酶法转化为SCN -,硫氰酸盐的浓度上升得更慢。在大鼠模型中,ATCA的浓度并未明显高于基线,但在兔子(高达40倍的增加)和猪(高达3倍的增加)中迅速上升,然后迅速下降,通常遵循相对行为氰化物。大鼠皮下注射氰化物,表观半衰期(t1 / 2)被确定为1,510 min。给兔子静脉内施用氰化物,并确定t1 / 2为177分钟。猪静脉注射氰化物,t1 / 2确定为26.9分钟。大鼠的SCN - t1 / 2为3,010分钟,但由于SCN -浓度未达到最大值,因此未在兔子和猪中进行计算。兔子和猪的ATCA t1 / 2分别为40.7和13.9分钟,而不能自信地确定为大鼠。目前的研究表明,通过确定每种动物模型中氰化物和SCN -的显着升高,可以在暴露后不久验证氰化物的暴露;当ATCA的解毒途径很重要时,可以使用ATCA。

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