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首页> 外文期刊>Journal of Analytical Methods in Chemistry >HPLC Method for Quantification of Caffeine and Its Three Major Metabolites in Human Plasma Using Fetal Bovine Serum Matrix to Evaluate Prenatal Drug Exposure
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HPLC Method for Quantification of Caffeine and Its Three Major Metabolites in Human Plasma Using Fetal Bovine Serum Matrix to Evaluate Prenatal Drug Exposure

机译:HPLC法测定胎儿血浆中咖啡因及其三种主要代谢产物的含量,方法是使用胎牛血清基质评估产前药物暴露

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Caffeine is recognized as the first-line therapeutic agent for apnea of prematurity. The dosage regimen is 10?mg/kg loading dose and 2.5?mg/kg maintenance dose. However, the plasma concentration achieved, not always, is therapeutically useful. It makes necessary to increase the doses to reach plasma concentration up to 30 or 35?μg/mL or even higher to attain therapeutic effect. To study why neonates have these differences, and whether these effects are linked to prenatal caffeine exposure, we had to develop an analytical method for an accurate measurement of caffeine and metabolites concentration. The analysis was carried out using fetal bovine serum (FBS) as biological matrix in a high-performance liquid chromatography with an ultraviolet detector method. This method allows acceptable chromatographic resolution between analytes in 15 minutes. It was validated and proved to be linear in the 0.1–40?μg/mL range for caffeine, paraxanthine, theobromine, and theophylline in the same chromatographic analysis. Accuracy for quality control samples for intra- and interday assays was ranged from 96.5 to 105.2% and 97.1 to 106.2%. Precision had CV no more than 10% in all concentration levels for all analytes. No differences were observed between quantification in human and FBS. This method was applied to quantify plasma drug concentration in mothers and their newborns in a Mexican northeast population. In our study, we confirmed self-reported caffeine maternal intake in 85.2% (); meanwhile, in their newborn’s plasma, it was detected only in 78% (). Caffeine plasma concentrations in mother and newborn had a linear relationship, and no differences were observed between groups (mothers versus children). These results suggest that our analytical method and substitution of biological matrix was linear, precise, and accurate for caffeine quantification and could be used for measuring prenatal exposure and let us to study, in the future, concentration differences observed during apnea clinical treatment.
机译:咖啡因被认为是早产呼吸暂停的一线治疗剂。剂量方案为10?mg / kg负荷剂量和2.5?mg / kg维持剂量。然而,并非总是如此,所达到的血浆浓度在治疗上是有用的。为了达到治疗效果,有必要增加剂量使血浆浓度达到30或35?μg/ mL甚至更高。为了研究新生儿为何具有这些差异,以及这些影响是否与产前咖啡因暴露有关,我们必须开发一种分析方法来准确测量咖啡因和代谢产物的浓度。使用胎牛血清(FBS)作为生物基质,在高效液相色谱仪中通过紫外线检测器方法进行分析。该方法可在15分钟内在分析物之间实现可接受的色谱分离度。在相同的色谱分析中,咖啡因,对黄嘌呤,可可碱和茶碱的浓度在0.1–40μg / mL范围内线性有效。日间和日间分析的质量控制样品的准确性范围为96.5至105.2%和97.1至106.2%。对于所有分析物,精密度的CV在所有浓度水平下均不超过10%。在人和FBS定量之间未观察到差异。该方法用于量化墨西哥东北人口母亲及其新生儿的血浆药物浓度。在我们的研究中,我们确认自我报告的咖啡因母亲摄入量为85.2%();同时,在他们的新生儿血浆中,只有78%()被检测到。母亲和新生儿中的咖啡因血浆浓度呈线性关系,各组之间(母亲与儿童)未观察到差异。这些结果表明,我们的分析方法和生物基质的替代方法对咖啡因的定量分析是线性,精确和准确的,可用于测量产前暴露,并让我们研究将来在呼吸暂停临床治疗期间观察到的浓度差异。

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