Probing the molecular interactions between cholinium-based ionic liquids and insulin aspart: A combined computational and experimental study

离子液体 化学 圆二色性 分子 分子动力学 溶剂化 氢键 结晶学 人口 计算化学 有机化学 人口学 社会学 催化作用
作者
Vidya Sundaram,Ramakrishnan Nagasundara Ramanan,Manikandan Selvaraj,Nafees Ahemad,R. Vijayaraghavan,Douglas R. MacFarlane,Chien Wei Ooi
出处
期刊:International Journal of Biological Macromolecules [Elsevier BV]
卷期号:253: 126665-126665 被引量:3
标识
DOI:10.1016/j.ijbiomac.2023.126665
摘要

Despite extensive studies revealing the potential of cholinium-based ionic liquids (ILs) in protein stabilization, the nature of interaction between ILs' constituents and protein residues is not well understood. In this work, we used a combined computational and experimental approach to investigate the structural stability of a peptide hormone, insulin aspart (IA), in ILs containing a choline cation [Ch]+ and either dihydrogen phosphate ([Dhp]-) or acetate ([Ace]-) as anions. Although IA remained stable in both 1 M [Ch][Dhp] and 1 M [Ch][Ace], [Dhp]- exhibited a much stronger stabilization effect than [Ace]-. Both the hydrophilic ILs intensely hydrated IA and increased the number of water molecules in IA's solvation shell. Undeterred by the increased number of water molecules, the native state of IA's hydrophobic core was maintained in the presence of ILs. Importantly, our results reveal the importance of IL concentration in the medium which was critical to maintain a steady population of ions in the microenvironment of IA and to counteract the denaturing effect of water molecules. Through molecular docking, we confirm that the anions exert the dominant effect on the structure of IA, while [Ch]+ have the secondary influence. The computational results were validated using spectroscopic analyses (ultra-violet, fluorescence, and circular dichroism) along with dynamic light scattering measurements. The extended stability of IA at 30 °C for 28 days in 1 M [Ch][Dhp] and [Ch][Ace] demonstrated in this study reveals the possibility of stabilizing IA using cholinium-based ILs.
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