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Therapeutic monitoring of topiramate: evaluation of the saturable distribution between erythrocytes and plasma of whole blood using an optimized high-pressure liquid chromatography method.

机译:托吡酯的治疗性监测:使用优化的高压液相色谱法评估全血红细胞与血浆之间的饱和分布。

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Topiramate (TPM) reportedly binds in a saturable manner to erythrocytes but minimally to plasma proteins. Two studies were performed to evaluate this distribution phenomenon. In all studies, TPM was measured with a newly developed, optimized procedure that uses octyldecyl (C-18) solid phase sorbents disks/packed cartridges and a DB-1 methylsilicone capillary gas chromatography (GC) column. Between-run precision coefficients of variation (CVs) (n = 16) ranged from 3.6%-5.6% at concentrations from 3.0 to 15 microg/mL, with low limit of detection of 0.2 to 0.3 microg/mL. For the distribution studies, drug-free whole-blood specimens from five healthy adult volunteers were supplemented with TPM and used to test the influence of TPM concentration and HCT differences on the plasma/blood (P/B) distribution ratio of TPM. In study A, TPM concentration was varied (1-15 microg/mL) and HCT remained constant (40% +/- 5%). In study B, TPM (3 microg/mL) was added to blood specimens comprising a range of HCT values (20%-40%). Study A results were: mean TPM P/B ratios: 0%, 14.2% +/- 5%, 44.2% +/- 4%, 76% +/- 5.5% at 1, 3, 5, 15 microg/mL, respectively. Data between each group were statistically different (p < 0.001). Study B results were: mean TPM P/B ratio: 17.3% +/- 7.3%, 27.5% +/- 10.1%, 39.8% +/- 8% and 56.1% +/- 8.8% at HCT values of 40%, 32%, 26.5%, 20%, respectively. The TPM P/B ratio was significantly inversely correlated to HCT (r = -905, p < 0.001). TPM P/B partitioning was not temperature-dependent. Researchers concluded that the saturable binding of TPM to RBC is significant and is correlated to HCT. As a result, TPM in the plasma fraction of whole blood will increase when HCT decreases and as total TPM concentration in whole blood increases.
机译:据报道,托吡酯(TPM)以可饱和的方式与红细胞结合,但与血浆蛋白的结合最少。进行了两项研究以评估这种分布现象。在所有研究中,均采用新开发的优化程序对TPM进行了测量,该程序使用辛基癸基(C-18)固相吸附剂盘/填充柱和DB-1甲基硅氧烷毛细管气相色谱(GC)柱。批间精密度变异系数(CV)(n = 16)在3.0至15 microg / mL的浓度范围内为3.6%-5.6%,检测下限为0.2至0.3 microg / mL。对于分布研究,对来自五名健康成人志愿者的无毒全血标本补充了TPM,并用于测试TPM浓度和HCT差异对TPM血浆/血液(P / B)分布比的影响。在研究A中,TPM浓度变化(1-15 microg / mL),HCT保持恒定(40%+/- 5%)。在研究B中,将TPM(3 microg / mL)添加到包含一系列HCT值(20%-40%)的血液样本中。研究A结果为:1、3、5、15微克/毫升时,平均TPM P / B比:0%,14.2%+ /-5%,44.2%+ /-4%,76%+ /-5.5%,分别。各组之间的数据具有统计学差异(p <0.001)。研究B结果为:在40%的HCT值下,平均TPM P / B比:17.3%+/- 7.3%,27.5%+/- 10.1%,39.8%+/- 8%和56.1%+/- 8.8%, 32%,26.5%,20%。 TPM P / B比与HCT呈显着负相关(r = -905,p <0.001)。 TPM P / B分区与温度无关。研究人员得出结论,TPM与RBC的饱和结合非常重要,并且与HCT相关。结果,当HCT降低时,随着全血中总TPM浓度的增加,全血中血浆中的TPM将增加。

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