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镧(III)对植物玻连蛋白样蛋白的影响及其毒理学基础的初步研究

A preliminary study on the effects of lanthanum (III) on plant vitronectin-like protein and its toxicological basis.

作者信息

Wang Lihong, He Jingfang, Yang Qing, Li Xiaodong, Wei Haiyan, Chen David D Y, Huang Xiaohua

机构信息

Jiangsu Collaborative Innovation Center of Biomedical Functional Materials, Jiangsu Key Laboratory of Biomedical Materials, School of Chemistry and Materials Science, Nanjing Normal University, Nanjing 210046, China; State Key Laboratory of Food Science and Technology, School of Environment and Civil Engineering, Jiangnan University, Wuxi 214122, China.

Jiangsu Collaborative Innovation Center of Biomedical Functional Materials, Jiangsu Key Laboratory of Biomedical Materials, School of Chemistry and Materials Science, Nanjing Normal University, Nanjing 210046, China.

出版信息

Ecotoxicol Environ Saf. 2017 Nov;145:227-234. doi: 10.1016/j.ecoenv.2017.07.039. Epub 2017 Jul 21.

Abstract

Vitronectin-like protein (VN) is widely found outside plant plasma membranes. The VN molecular surface contains a large number of active groups that combine strongly with rare earth elements (REEs), which means that VN is a preferential binding target for REEs exhibiting their toxic effects, but the toxicological mechanism remains unknown. This study used transmission electron microscopy, circular dichroism, fluorescence spectrometry, ultraviolet-visible spectroscopy, X-ray photoelectron spectroscopy, and calculational chemistry (homology modeling, molecular dynamics simulation and quantum chemical calculation) to preliminarily investigate the effect of lanthanum [La(III)] as an REE, on the structure of VN and its toxicological mechanism. The results showed that low-concentration La(III) could cause micro-interference to the VN molecular structure through weak interactions, such as electrostatic attraction. High-concentration La(III) formed stable complexes with VN, which changed the average binding energy and electron cloud density of VN, loosened the molecular structure and increased the disorder of VN molecule. The results of building a 3D model of VN and simulating the interaction between La(III) and VN using calculational chemistry showed that La(HO) in solution could coordinately bind to the carboxyl-/carbonyl-O groups in the negatively charged areas on the VN molecular surface. Furthermore, one or more strong H-bonds were formed to enhance the stability of the La(HO)-VN complexes. In summary, low La(III) concentrations could cause micro-interference to the VN molecular structure, whereas high La(III) concentrations could coordinately bind to VN to form stable La-VN complexes, which destroyed the molecular structure of VN; thus the toxicological basis by which La(III) exhibits its toxic effects is its binding to VN.

摘要

玻连蛋白样蛋白(VN)广泛存在于植物质膜外。VN分子表面含有大量与稀土元素(REEs)强烈结合的活性基团,这意味着VN是REEs发挥毒性作用的优先结合靶点,但其毒理学机制尚不清楚。本研究利用透射电子显微镜、圆二色性、荧光光谱、紫外可见光谱、X射线光电子能谱以及计算化学(同源建模、分子动力学模拟和量子化学计算)初步研究了作为REEs的镧[La(III)]对VN结构的影响及其毒理学机制。结果表明,低浓度的La(III)可通过静电吸引等弱相互作用对VN分子结构造成微扰。高浓度的La(III)与VN形成稳定的复合物,改变了VN的平均结合能和电子云密度,使分子结构松弛,增加了VN分子的无序性。利用计算化学构建VN的三维模型并模拟La(III)与VN之间的相互作用结果表明,溶液中的La(HO)可与VN分子表面带负电区域的羧基/羰基-O基团配位结合。此外,还形成了一个或多个强氢键以增强La(HO)-VN复合物的稳定性。综上所述,低浓度的La(III)可对VN分子结构造成微扰,而高浓度的La(III)可与VN配位结合形成稳定的La-VN复合物,破坏VN的分子结构;因此,La(III)发挥毒性作用的毒理学基础是其与VN的结合。

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