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首页> 外文期刊>Electrophoresis: The Official Journal of the International Electrophoresis Society >Capillary electrophoresis for determination of free and albumin-bound bilirubin and the investigation of drug interaction with bilirubin-bound albumin
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Capillary electrophoresis for determination of free and albumin-bound bilirubin and the investigation of drug interaction with bilirubin-bound albumin

机译:毛细管电泳测定游离和结合白蛋白的胆红素以及与结合胆红素的药物相互作用的研究

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Capillary electrophoresis (CE) is a promising technique for assessment of free bilirubin and its interaction with albumin, as it requires only a small sample volume and provides a rapid and efficient separation of free bilirubin from its albumin-bound complex in a one-phase system. In order to maintain the equilibrium without dissociation of bilirubin from the albumin/bilirubin complex as in real clinical conditions, the coupling of CE with frontal analysis (FA) was investigated. A very large sample plug was introduced hydrodynamically into the capillary (36 cm length, 50 mu m inner diameter) at 15 psi.s to develop the frontal conditions during CE separation. The working conditions for CE/FA separation of bilirubin and albumin were optimized as follows: +20 kV; running buffer, 10 mmol/L phosphate and 1 mmol/L ethylenediaminetetraacetic acid (EDTA), pH 7.4. The working range for bilirubin was found to vary from 5 to 206 mu mol/L; precision with relative standard deviation (RSD) <2.0% for n = 3 and detection limit (signal to noise, S/N = 2) was 2 mu mol/L. The residual binding capacity of a simulated cord blood serum for bilirubin was 26 mg/100 mL at pH 7.4. Bilirubin was shown to be displaced from albumin when aspirin was added. The free bilirubin concentration was found to increase to clinical significant concentrations from 11.9 to 21.1% when increasing aspirin was added in the range of 5-50 mg/100 mL, respectively. Thus, the investigation of aspirin displacement of bilirubin from albumin is clinically important and the CE/FA method is a suitable procedure for this purpose. [References: 25]
机译:毛细管电泳(CE)是一种评估游离胆红素及其与白蛋白相互作用的有前途的技术,因为它仅需少量样品即可在一个单相系统中快速,有效地将游离胆红素从其结合白蛋白的复合物中分离出来。为了在实际临床条件下保持平衡而不使胆红素从白蛋白/胆红素复合物中解离,我们研究了CE与额叶分析(FA)的耦合。在15 psi.s的压力下将一个非常大的样品塞以流体力学方式引入毛细管(36 cm长,内径50μm内径)中,以在CE分离过程中产生正面条件。 CE / FA分离胆红素和白蛋白的工作条件优化如下:+20 kV;运行缓冲液,10 mmol / L磷酸盐和1 mmol / L乙二胺四乙酸(EDTA),pH 7.4。胆红素的工作范围为5至206μmol / L。相对标准偏差(RSD)<2.0%(n = 3)和检测限(信号噪声,S / N = 2)的精密度为2μmol / L。在pH 7.4下,模拟脐带血血清对胆红素的残留结合能力为26 mg / 100 mL。添加阿司匹林后,胆红素已从白蛋白中置换出来。当分别在5-50 mg / 100 mL范围内添加增加的阿司匹林时,发现游离胆红素浓度从11.9%增至21.1%的临床显着浓度。因此,研究阿司匹林从白蛋白置换胆红素的临床意义是重要的,CE / FA方法是实现此目的的合适方法。 [参考:25]

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