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The interaction of beta-lactoglobulin with ciprofloxacin and kanamycin; a spectroscopic and molecular modeling approach

化学 卡那霉素 圆二色性 对接(动物) 假名 荧光光谱法 荧光 结合位点 生物物理学 蛋白质二级结构 环丙沙星 生物化学 抗生素 生物 汉字 护理部 哲学 物理 汉字 医学 量子力学 语言学
作者
Mohammad Hossein Mehraban,Salman Odooli,Reza Yousefi,Rasoul Roghanian,Majid Motovali-Bashi,Ali Akbar Moosavi–Movahedi,Younes Ghasemi
出处
期刊:Journal of Biomolecular Structure & Dynamics [Taylor & Francis]
卷期号:35 (9): 1968-1978 被引量:17
标识
DOI:10.1080/07391102.2016.1203819
摘要

A vast research has been conducted to find suitable and safe carriers for vital and pH-sensitive drugs including antibiotics. This article reports the use of easily accessible and abundant purified beta-lactoglobulin (β-LG) protein as the potential carrier of widely used Kanamycin (Kana) and Ciprofloxacin (Cip) antibiotics. Spectroscopic techniques (Fluorescence, UV-vis, Circular Dichroism) combined with molecular docking were used to determine the binding mechanism of these drugs. Fluorescence studies showed moderate binding affinity with the calculated binding constants KCip = 60.1 (±0.2) × 103 M-1 and Kkana = 2.5 (±0.6) × 103 M-1 with the order of Cip > Kana. Results of UV-vis were consistent with fluorescence measurements and demonstrated a stronger complexation for Cip rather than Kana. The secondary structure of β-LG was preserved upon interaction with Kana; however, a reduction in β-sheet content from 39.1 to 31.9% was convoyed with an increase in α-helix from 12.8 to 20.5% due to complexation of Cip. Molecular docking studies demonstrated that preferred binding sites of these drugs are not the same and several amino acids are involved in stabilizing the interaction. Based on the achieved results, Kana and Cip can spontaneously bind to β-LG and this protein may serve as their transport vehicle.
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