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一种用于尿液样本中吗啡预浓缩的新型肽基微萃取纤维的分子模拟与实验研究

Molecular modeling and experimental study of a new peptide-based microextraction fiber for preconcentrating morphine in urine samples.

作者信息

Riahi-Zanjani Bamdad, Balali-Mood Mahdi, Es'haghi Zarrin, Asoodeh Ahmad, Ghorani-Azam Adel

机构信息

Medical Toxicology Research Center, Mashhad University of Medical Sciences, Mashhad, Iran.

Medical Toxicology and Drug Abuse Research Center, Birjand University of Medical Sciences, Birjand, Iran.

出版信息

J Mol Model. 2019 Feb 8;25(3):54. doi: 10.1007/s00894-019-3925-7.

Abstract

Antimicrobial peptides (AMPs) are best known for their bactericidal properties; however, due to their unique and flexible structures, they have also been proposed as potential selective sorbents for specific molecules. In the present study, we aimed to design and produce a new peptide-based microextraction fiber for preconcentrating morphine in urine samples. The binding of morphine to the peptide was first evaluated by computational simulation using the Molecular Operating Environment (MOE) 2015.10 software. A similar study was then performed using DS BIOVIA Materials Studio 2017 v17.1.0.48, which confirmed the results of the simulation carried out with MOE. Afterwards, those results were also confirmed by experimental research. In the experimental evaluation, carbon nanotubes (CNTs) were initially carboxylated with HSO/HNO (3:1) and then functionalized with the peptide. FTIR analysis, Raman measurements, and SEM imaging were used to confirm that CNT functionalization was successful as well as to check the nanostructure of the fiber. To evaluate the functionality of the fiber, it was inserted into a microtube containing a urine sample that included morphine and then sonicated for 5 min at 40 °C. Afterwards, the fiber was washed with methanol 20% (HO/methanol) and the resulting sample was analyzed by HPLC. This procedure was repeated for different concentrations of morphine in the urine sample. The computational and experimental results showed that a morphine concentration as low as 0.25 ppb in urine could be adsorbed and detected using the peptide fiber. Therefore, given its semi-selective binding affinity for morphine, this peptide-based fiber can be considered a new approach to the detection of small amounts of morphine in biological samples.

摘要

抗菌肽(AMPs)以其杀菌特性而闻名;然而,由于其独特且灵活的结构,它们也被提议作为特定分子的潜在选择性吸附剂。在本研究中,我们旨在设计并制备一种新型的基于肽的微萃取纤维,用于尿液样本中吗啡的预浓缩。首先使用分子操作环境(MOE)2015.10软件通过计算模拟评估吗啡与该肽的结合情况。随后使用DS BIOVIA Materials Studio 2017 v17.1.0.48进行了类似研究,证实了用MOE进行的模拟结果。之后,这些结果也通过实验研究得到了证实。在实验评估中,碳纳米管(CNTs)首先用HSO/HNO(3:1)进行羧基化,然后用该肽进行功能化。使用傅里叶变换红外光谱(FTIR)分析、拉曼测量和扫描电子显微镜(SEM)成像来确认CNT功能化是否成功以及检查纤维的纳米结构。为了评估纤维的功能,将其插入含有吗啡的尿液样本的微管中,然后在40℃下超声处理5分钟。之后,用20%的甲醇(水/甲醇)洗涤纤维,所得样品通过高效液相色谱(HPLC)进行分析。对尿液样本中不同浓度的吗啡重复此过程。计算和实验结果表明,使用该肽纤维可以吸附并检测尿液中低至0.25 ppb的吗啡浓度。因此,鉴于其对吗啡的半选择性结合亲和力,这种基于肽的纤维可被视为检测生物样本中少量吗啡的一种新方法。

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