Inhibition of voltage-gated sodium ion channel by corannulene and computational inversion blockage underlying mechanisms

化学 生物物理学 PEG比率 离子通道 离子 钠通道 纳米材料 纳米技术 材料科学 生物化学 有机化学 受体 生物 财务 经济
作者
Xiaoxia Zuo,Hongqiang Yin,Xinyu Li,Zhenzhen Jia,Yanlei Wang,Zhuo Yang,Xisheng Feng
出处
期刊:Biochemical and Biophysical Research Communications [Elsevier BV]
卷期号:656: 70-77
标识
DOI:10.1016/j.bbrc.2023.03.042
摘要

Corannulene (Cor), a special carbon material, evidenced strong protein binding capacity which regulating lysozyme crystallization and controlling reactive oxygen species (ROS) generation. Ion channel protein play role in regulating ion channel functions to affect physiological functions. However, the interaction between Cor and ion channel protein have not been studied. In this study, PEG/Cor nanoparticles (PEG/Cor Nps) were prepared by mPEG-DSPE. The PEG/Cor Nps localized in cytoplasm and produced cytotoxicity at high concentration. Whole cell patch clamp examined ion channel functions after incubate PEG/Cor Nps with PC-12 cell. we found that PEG/Cor Nps inhibited voltage-gated Na+ ion channels in a dose- and time-dependent manner but not act on voltage-gated K+ ion channels. The potential mechanisms were revealed by all-atom molecular dynamic (MD) simulations. The results showed that PEG/Cor Nps block the pore of sodium ion channel protein due to dose- and time-dependent accumulation. Besides, the orientation angle (θ) configuration of PEG/Cor Nps will be inverted with the accumulation to generate two blocking mechanisms. Different from other carbon nanomaterials, the blockage mechanism of PEG/Cor Nps provides novel insights into the mechanisms of interaction between carbon nanomaterials and protein.

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