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首页> 外文期刊>Journal of Analytical Toxicology >Simultaneous Measurement of 3-Chlorotyrosine and 3,5-Dichlorotyrosine in Whole Blood, Serum and Plasma by Isotope Dilution HPLC-MS-MS
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Simultaneous Measurement of 3-Chlorotyrosine and 3,5-Dichlorotyrosine in Whole Blood, Serum and Plasma by Isotope Dilution HPLC-MS-MS

机译:同位素稀释HPLC-MS-MS同时测定全血,血清和血浆中的3-氯代酪氨酸和3,5-二氯酪氨酸

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Chlorine is a public health concern and potential threat due to its high reactivity, ease and scale of production, widespread industrial use, bulk transportation, massive stockpiles and history as a chemical weapon. This work describes a new, sensitive and rapid stable isotope dilution method for the retrospective detection and quantitation of two chlorine adducts. The biomarkers 3-chlorotyrosine (Cl-Tyr) and 3,5-dichlorotyrosine (Cl-2-Tyr) were isolated from the pronase digest of chlorine exposed whole blood, serum or plasma by solid-phase extraction (SPE), separated by reversed-phase HPLC and detected by tandem mass spectrometry (MS-MS). The calibration range is 2.50-1,000 ng/mL (R-2 a parts per thousand yen 0.998) with a lowest reportable limit (LRL) of 2.50 ng/mL for both analytes, an accuracy of a parts per thousand yen93% and an LOD of 0.443 ng/mL for Cl-Tyr and 0.396 ng/mL for Cl-2-Tyr. Inter- and intra-day precision of quality control samples had coefficients of variation of a parts per thousand currency sign10% and a parts per thousand currency sign7.0%, respectively. Blood and serum samples from 200 healthy individuals and 175 individuals with chronic inflammatory disease were analyzed using this method to assess background levels of chlorinated tyrosine adducts. Results from patients with no known inflammatory disease history (healthy) showed baseline levels of < LRL-4.26 ng/mL Cl-Tyr and < LRL Cl-2-Tyr. Patients with inflammatory disease had baseline levels of < LRL-15.4 ng/mL Cl-Tyr and < LRL-5.22 ng/mL Cl-2-Tyr. Blood exposed to 2.02 ppm chlorine gas for 15 min produced 941 ng/mL Cl-Tyr and 223 ng/mL Cl-2-Tyr. This high-throughput method has been developed and analytically validated for the diagnosis of human exposure to chlorine.
机译:氯由于其高反应性,易于生产和规模化,广泛的工业用途,大量运输,大量库存和化学武器的历史而成为公共卫生关注和潜在威胁。这项工作描述了一种新的,灵敏的,快速稳定的同位素稀释方法,用于追溯检测和定量两种氯加合物。通过固相萃取(SPE)从暴露于氯的全血,血清或血浆的链霉蛋白酶消化物中分离出生物标志物3-氯酪氨酸(Cl-Tyr)和3,5-二氯酪氨酸(Cl-2-Tyr),通过反相分离相HPLC并通过串联质谱(MS-MS)检测。校准范围为2.50-1,000 ng / mL(R-2千分之几为0.998),两种分析物的最低报告限(LRL)为2.50 ng / mL,千分之几的准确度为93%和LOD Cl-Tyr为0.443 ng / mL,Cl-2-Tyr为0.396 ng / mL。质量控制样品的日间和日内精度分别具有千分之一货币符号的变化系数10%和千分之一货币符号的变化系数7.0%。使用这种方法分析了200名健康个体和175名患有慢性炎性疾病的个体的血液和血清样本,以评估氯化酪氨酸加合物的背景水平。没有已知炎性疾病病史(健康)的患者的结果显示,基线水平为

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