RESUMO
Objective To investigate the maximum allowable deviation of ion abundance ratios of characteristic fragment ions in common drugs (poisons) in blood by gas chromatography-mass spectrometry (GC-MS) method. Methods Four common drugs (poisons) (dichlorvos, phorate, diazepam and estazolam) were detected by GC-MS full scan mode after liquid-liquid extraction in two laboratories and under three chromatographic conditions. The deviations of ion abundance ratios of the four common drugs (poisons) in marked blood samples with concentrations of 0.5, 1.0, 2.0, 5.0 and 10.0 μg/mL were analyzed. At the same time, the false negative rates of ion abundance ratios were analyzed when the mass concentration was limit of detection (LOD), 2LOD, limit of quantitation (LOQ) and 2LOQ, and the false positive rates of ion abundance ratios were analyzed with blank blood samples. Results Under the two laboratories, four common drugs (poisons) and three kinds of chromatography conditions, the differences in deviations of the ion abundance ratios of marked blood samples were not statistically significant (P>0.05). More than 95% of the absolute deviations of the ion abundance ratios of the marked blood samples were within the range of ±10%, and more than 95% of the relative deviations were within the range of ±25%. In cases of low concentration (concentration less than 2LOQ) or low signal to noise ratio (3-15), the false negative rate was less than 5% and the false positive rate was 0% when the relative deviation was greater than 50%. Conclusion The absolute deviations of ion abundance ratios of four common drugs (poisons) in marked blood samples are advised to have a determination range within ±10%, and the determination range of relative deviations within ±25%.
Assuntos
Humanos , Cromatografia Gasosa-Espectrometria de Massas , Íons/química , Limite de Detecção , Extração Líquido-Líquido , Venenos/sangueRESUMO
El contacto con el veneno de la oruga Lonomia achelous produce en humanos un síndrome hemorrágico, debido a alteraciones en la hemostasis. Los estudios de coagulación y fibrinolisis de los pacientes mostraron, como signos constantes, disminución del fibrinógeno,plasminógeno, factor XIII y aparición de FDP en el suero, y en las necropsias hemorragias generalizadas. Con el objeto de obtener mayor información sobre el mecanismo "in vitro" de ese veneno, tratamos de reproducir en conejos, el síndrome hemorrágico descrito en humanos. Para ello, se determinaron los valores normales de los diversos factores de la coagulación en esa especie, y el efecto que causan las extracciones sucesivas de sangre sobre la concentración de esos factores. Como resultado, se encontró un rango de valores muy amplio para el fibrinógeno, una concentración muy elevada del factor V y menos pronunciada en los factores XIII y X; no se demostró actividad fibrinolítica en el plasma, ni en la fracción euglobulina médica en placas de fibrina; tampoco se detectaron en el suero. Las extracciones sucesivas de sangre produjeron variabilidad en las concentraciones de fibrinógeno, plasminógeno, protrombina y factor X con tendencia a valores por encima de los basales