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首页> 外文期刊>Chemical and Pharmaceutical Bulletin >A Simple High-Throughput Method for Determination of Antiepileptic Analogues of γ-Aminobutyric Acid in Pharmaceutical Dosage Forms Using Microplate Fluorescence Reader
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A Simple High-Throughput Method for Determination of Antiepileptic Analogues of γ-Aminobutyric Acid in Pharmaceutical Dosage Forms Using Microplate Fluorescence Reader

机译:使用微孔板荧光读取器测定药物剂型中γ-氨基丁酸的抗癫痫药类似物的简单高通量方法

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摘要

Pregabalin (PGB), gabapentin (GBP), and vigabatrin (VGB) are structural analogues of γ-aminobutyric acid used for the treatment of different forms of epilepsy. Their analytical determination is challenging since these molecules have no significant UV or visible absorption. Several derivatization methods have been developed and used for their determination in bulk or pharmaceutical dosage forms. We aimed to develop a high-throughput method using a microplate reader with fluorescence detection and simple derivatization with fluorescamine. Obtained method involves derivatization step of only 5 min at room temperature and simultaneous measurements of 96 samples (λ_(ex) 395, λ_(em) 476 nm) thus rendering excellent high-throughput analysis. The method was found to be linear with r~2>0. 998 across investigated analytical ranges of 0. 75 to 30. 0μg/ mL for PGB, 2. 00 to 80. 0μg/mL for GBP, and 1. 50 to 60. 0/μg/mL for VGB. Intraday and interday precision values did not exceed 4. 93%. The accuracy was ranging between 96. 6 to 103. 5%. The method was also found to be specific since used excipients did not interfere with the method. The robustness study showed that derivatization procedure is more robust than spectrofluorimetric conditions. The developed high-throughput, method was successfully applied for determination of drug content and dissolution profiles in pharmaceutical dosage forms of studied antiepileptic drugs.
机译:普瑞巴林(PGB),加巴喷丁(GBP)和vigabatrin(VGB)是用于治疗不同形式癫痫病的γ-氨基丁酸的结构类似物。由于这些分子没有明显的紫外线或可见光吸收,因此其分析测定具有挑战性。已经开发了几种衍生化方法,并将其用于散装或药物剂型的测定。我们旨在开发一种使用酶标仪的高通量方法,该酶标仪具有荧光检测功能和简单的荧光胺衍生作用。获得的方法仅需在室温下进行5分钟的衍生化步骤,即可同时测量96个样品(λ_(ex)395,λ_(em)476 nm),从而提供出色的高通量分析。发现该方法是线性的,r〜2> 0。 998的研究分析范围为PGB为0. 75至30.0μg/ mL,GBP为2. 00至80.0μg/ mL,VGB为1. 50至60. 0 /μg/ mL。日内和日间精度值不超过4。93%。准确性介于96. 6至103. 5%之间。还发现该方法是特异性的,因为使用的赋形剂不会干扰该方法。鲁棒性研究表明,衍生化过程比荧光光谱法更鲁棒。所开发的高通量方法已成功地用于确定所研究的抗癫痫药的药物剂型中的药物含量和溶出度。

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