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Toxicokinetics including saturable protein binding of 4-chloro-2-methyl phenoxyacetic acid (MCPA) in patients with acute poisoning

机译:急性中毒患者的4-氯-2-甲基苯氧基乙酸(MCPA)的毒性动力学包括饱和蛋白结合

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摘要

Human data on protein binding and dose-dependent changes in toxicokinetics for MCPA are very limited. 128 blood samples were obtained in 49 patients with acute MCPA poisoning and total and unbound concentrations of MCPA were determined. The Scatchard plot was biphasic suggesting protein binding to two sites. The free MCPA concentration increased when the total concentration exceeded 239 mg/L (95% confidence interval 198–274 mg/L). Nonlinear regression using a two-site binding hyperbola model estimated saturation of the high affinity binding site at 115 mg/L (95%CI 0–304). Further analyses using global fitting of serial data and adjusting for the concentration of albumin predicted similar concentrations for saturable binding (184 mg/L and 167 mg/L, respectively) without narrowing the 95%CI. In 25 patients, the plasma concentration–time curves for both bound and unbound MCPA were approximately log-linear which may suggest first order elimination, although sampling was infrequent so zero order elimination cannot be excluded. Using a cut-off concentration of 200 mg/L, the half-life of MCPA at higher concentrations was 25.5 h (95%CI 15.0–83.0 h; n = 16 patients) compared to 16.8 h (95%CI 13.6–22.2 h; n = 10 patients) at lower concentrations. MCPA is subject to saturable protein binding but the influence on half-life appears marginal.
机译:关于MCPA的蛋白质结合和毒性动力学的剂量依赖性变化的人类数据非常有限。在49例急性MCPA中毒患者中采集了128份血样,并确定了MCPA的总浓度和未结合浓度。斯卡查德图是双相的,表明蛋白质与两个位点结合。当总浓度超过239 mg / L(95%置信区间198-274 mg / L)时,游离MCPA浓度增加。使用两点结合双曲线模型的非线性回归估计高亲和力结合位点的饱和度为115 mg / L(95%CI 0–304)。使用序列数据的全局拟合并调整白蛋白浓度进行的进一步分析预测可饱和结合的相似浓度(分别为184 mg / L和167 mg / L),而不会缩小95%CI。在25例患者中,结合的和未结合的MCPA的血浆浓度-时间曲线大致呈对数线性,这可能表明一阶消除,尽管采样很少,因此不能排除零阶消除。使用200 mg / L的截断浓度,较高浓度时MCPA的半衰期为25.5 h(95%CI 15.0-83.0 h; n = 16位患者),而16.8 h(95%CI 13.6-22.2 h ; n = 10位患者)。 MCPA受到饱和蛋白质结合的影响,但对半衰期的影响似乎很小。

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