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与托吡酯结合后人类碳酸酐酶 II 的本征荧光增强:一些关于药物诱导蛋白质分子收缩的证据。

Enhancement of intrinsic fluorescence of human carbonic anhydrase II upon topiramate binding: Some evidence for drug-induced molecular contraction of the protein.

机构信息

Department of Biology, Faculty of Science, Razi University, 67149-67346, Kermanshah, Iran.

Department of Biology, Faculty of Science, Razi University, 67149-67346, Kermanshah, Iran.

出版信息

Int J Biol Macromol. 2018 Mar;108:240-249. doi: 10.1016/j.ijbiomac.2017.12.011. Epub 2017 Dec 5.

DOI:10.1016/j.ijbiomac.2017.12.011
PMID:29217181
Abstract

In this report, the effect of topiramate (TPM), an anticonvulsant sulfamate drug, on the structure of human carbonic anhydrase II (hCA II) was investigated by spectroscopic techniques. The intrinsic fluorescence experiments indicated that TPM binding causes enhancement of enzyme fluorescence via decreasing the internal quenching and energy transfer efficiency, the result supported by molecular dynamics simulation. Thermodynamic analysis of the binding process suggested that hydrogen bonding and van der Waals interactions are the major forces in the interaction of TPM with hCA II. The far-UV circular dichroism (CD) results showed that TPM caused increment in α-helical and β-sheet content of hCA II whereas, near-UV CD experiments in the presence of the drug showed induction of some compactness in the enzyme tertiary structure. The number of accessible tryptophans and protein surface hydrophobicity index of the enzyme were reduced in the presence of TPM which confirms the enzyme structural compactness upon drug binding. In addition, the enzyme thermal stability was increased in the presence of the drug. It seems that the induction of compactness in the enzyme structure upon drug binding may be responsible for increment of its conformational stability.

摘要

本报告采用光谱技术研究了抗惊厥磺胺类药物托吡酯(TPM)对人碳酸酐酶 II(hCA II)结构的影响。荧光实验表明,TPM 结合通过降低内部猝灭和能量转移效率增强了酶的荧光,分子动力学模拟的结果支持了这一结论。结合过程的热力学分析表明,氢键和范德华相互作用是 TPM 与 hCA II 相互作用的主要力。远紫外圆二色性(CD)结果表明,TPM 导致 hCA II 的α-螺旋和β-折叠含量增加,而在药物存在下的近紫外 CD 实验表明,酶的三级结构诱导了一些紧凑性。在 TPM 的存在下,酶的可及色氨酸数量和蛋白质表面疏水性指数减少,这证实了药物结合时酶结构的紧凑性。此外,在药物存在下,酶的热稳定性增加。似乎是药物结合诱导酶结构的紧凑性增加,导致其构象稳定性增加。

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