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带负电荷的神经节苷脂促进两亲性神经递质的膜结合。

Negatively Charged Gangliosides Promote Membrane Association of Amphipathic Neurotransmitters.

机构信息

Laboratory of Physics, Tampere University of Technology, P.O. Box 692, FI-33101 Tampere, Finland.

University of Jyvaskyla, Computational Bioscience Laboratory, Department of Biological and Environmental Science & Nanoscience Center, P.O. Box 35, FI-40014 University of Jyvaskyla, Finland.

出版信息

Neuroscience. 2018 Aug 1;384:214-223. doi: 10.1016/j.neuroscience.2018.05.035. Epub 2018 Jun 1.

Abstract

Lipophilic neurotransmitters (NTs) such as dopamine are chemical messengers enabling neurotransmission by adhering onto the extracellular surface of the post-synaptic membrane in a synapse, followed by binding to their receptors. Previous studies have shown that the strength of the NT-membrane association is dependent on the lipid composition of the membrane. Negatively charged lipids such as phosphatidylserine, phosphatidylglycerol, and phosphatidic acid have been indicated to promote NT-membrane binding, however these anionic lipids reside almost exclusively in the intracellular leaflet of the post-synaptic membrane instead of the extracellular leaflet facing the synaptic cleft. Meanwhile, the extracellular leaflet is relatively rich in biologically relevant anionic gangliosides such as monosialotetrahexosylganglioside (GM1), yet the role of gangliosides in NT-membrane association is not clear. Here, we explored the role of GM1 in modulating the binding of dopamine and histamine (as amphipathic/cationic NTs) as well as acetylcholine (as a hydrophilic/cationic NT) with the post-synaptic membrane surface. Atomistic molecular dynamics simulations and free energy calculations indicated that GM1 fosters membrane association of histamine and dopamine. For acetylcholine, this effect was not observed. The in silico results suggest that gangliosides form a charge-based vestibule in front of the post-synaptic membrane, attracting amphipathic NTs to the vicinity of the membrane. The results also stress the importance to understand the significance of the structural details of NTs, as exemplified by the GM1-acetylcholine interaction. In a larger context, the NT-membrane adherence, coupled to lateral diffusion in the membrane plane, is proposed to improve neurotransmission efficiency by advancing NT entry into the membrane-embedded ligand-binding sites.

摘要

亲脂性神经递质(NTs),如多巴胺,是化学信使,通过黏附在突触后膜的细胞外表面来实现神经传递,然后与受体结合。先前的研究表明,NT 与膜的亲和力取决于膜的脂质组成。带负电荷的脂质,如磷脂酰丝氨酸、磷脂酰甘油和磷脂酸,已被证明可以促进 NT 与膜的结合,然而这些阴离子脂质几乎只存在于突触后膜的胞质小叶,而不是面向突触间隙的细胞外小叶。同时,细胞外小叶富含生物学上相关的阴离子神经节苷脂,如单唾液酸四己糖神经节苷脂(GM1),但神经节苷脂在 NT 与膜的结合中的作用尚不清楚。在这里,我们探讨了 GM1 在调节多巴胺和组胺(作为两亲性/阳离子 NTs)以及乙酰胆碱(作为亲水性/阳离子 NT)与突触后膜表面结合中的作用。原子分子动力学模拟和自由能计算表明,GM1 促进了组胺和多巴胺与膜的结合。对于乙酰胆碱,没有观察到这种效果。计算机模拟结果表明,神经节苷脂在突触后膜前面形成一个基于电荷的前庭,吸引两亲性 NT 靠近膜。结果还强调了理解 NT 结构细节的重要性,GM1-乙酰胆碱相互作用就是一个很好的例子。从更大的角度来看,NT 与膜的黏附,加上在膜平面内的侧向扩散,被认为可以通过促进 NT 进入膜内配体结合位点来提高神经传递效率。

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