Synthesis of Molecularly Imprinted Polymers for Selective Extraction Followed by Solid Phase Determination of Metformin in Pharmaceutical Preparation and in Human Serum

IF 1.2 Q3 MULTIDISCIPLINARY SCIENCES Baghdad Science Journal Pub Date : 2023-10-20 DOI:10.21123/bsj.2023.8225
Rana A. Kamal Aldeen, Yehya K. Al-Bayati
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Abstract

This paper demonstrates that the synthesising and storage of molecular-imprinted polymers (MIP) at room temperature using bulk polymerisation of Metformin (Met) is characterised by high sensitivity, reduced costs, increased stability, and extended life. The research used 0.8:4:20 mmol ratios of template, monomer and cross-linking agents for the polymerisation in order to ensure an appropriate adsorption capacity. Benzoyl peroxide BPO was employed as the initiator for the functional monomer styrene C8H8 , cross-linked with Ethylene glycol dimethacrylate EGDMA C10H14O4, thereby creating MIP for Metformin(Met-MIP) that could be characterised with UV-Visible Spectrophotometry at 236nm, for pharmaceutical drugs and human serum. Fourier-transform infrared spectroscopy (FTIR) and scanning electron microscopy (SEM) was used for MIP drug. The elution process that was applied to the template (Met.) from the Met-MIP created cavities that were caused by the porogenic mixture solvents that were created from methanol, chloroform and acetic acid (70:20:10) mL respectively. The maximum adsorption capacity was 1.2320, 2.4448 µmol/g for two studies using 0.1 and 0.2 g weights of Met-MIP respectively. A solid-phase extraction (SPE) syringe packed with molecular imprinted polymers (MIPs) was employed to selectively separate and pre-concentrate the Metformin in multiple pharmaceutical drugs from several sources. The human serum was based on the use of deionized water to dilute the serum, followed by the heating of the serum with methanol. Subsequently, a few drops hydrochloric acid 1M were applied to gate transparence solution and detect Metformin at UV region 236 nm by applying the standard addition method.
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分子印迹聚合物的合成及其固相法测定药物制剂和人血清中二甲双胍的含量
本文证明了利用二甲双胍(Met)的体聚合在室温下合成和储存分子印迹聚合物(MIP)的特点是灵敏度高,成本低,稳定性高,寿命长。本研究采用0.8:4:20 mmol比例的模板、单体和交联剂进行聚合,以保证合适的吸附量。过氧化苯甲酰BPO作为功能单体苯乙烯C8H8的引发剂,与乙二醇二甲基丙烯酸酯EGDMA C10H14O4交联,从而生成二甲双胍MIP (Met-MIP),该MIP可以用紫外可见分光光度法在236nm处进行表征,用于药物和人血清。采用傅里叶变换红外光谱(FTIR)和扫描电镜(SEM)对MIP药物进行分析。对Met- mip模板(Met.)的洗脱过程产生的空腔是由分别由甲醇、氯仿和乙酸(70:20:10)mL形成的致孔混合溶剂引起的。分别使用0.1和0.2 g质量的Met-MIP,最大吸附量分别为1.2320、2.4448µmol/g。采用分子印迹聚合物(MIPs)填充固相萃取(SPE)注射器,对不同来源的多种药物中的二甲双胍进行选择性分离和预浓缩。人血清是基于使用去离子水稀释血清,然后用甲醇加热血清。随后,在门式透明溶液中滴入少量盐酸1M,在紫外区236 nm处采用标准加成法检测二甲双胍。
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来源期刊
Baghdad Science Journal
Baghdad Science Journal MULTIDISCIPLINARY SCIENCES-
CiteScore
2.00
自引率
50.00%
发文量
102
审稿时长
24 weeks
期刊介绍: The journal publishes academic and applied papers dealing with recent topics and scientific concepts. Papers considered for publication in biology, chemistry, computer sciences, physics, and mathematics. Accepted papers will be freely downloaded by professors, researchers, instructors, students, and interested workers. ( Open Access) Published Papers are registered and indexed in the universal libraries.
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