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脂质膜与纳米结构表面的相互作用。

Interaction of lipid membrane with nanostructured surfaces.

作者信息

Roiter Yuri, Ornatska Maryna, Rammohan Aravind R, Balakrishnan Jitendra, Heine David R, Minko Sergiy

机构信息

Department of Chemistry and Biomolecular Science, NanoBio Laboratory (NABLAB), Clarkson University, Potsdam, New York 13699-5810, USA.

出版信息

Langmuir. 2009 Jun 2;25(11):6287-99. doi: 10.1021/la900119a.

Abstract

Tiny details of the phospholipid (DMPC) membrane morphology in close vicinity to nanostructured silica surfaces have been discovered in the atomic force microscopy experiments. The structural features of the silica surface were varied in the experiments by the deposition of silica nanoparticles of different diameter on plane and smooth silica substrates. It was found that, due to the barrier function of the lipid membrane, only particles larger than 22 nm in diameter with a smooth surface were completely enveloped by the lipid membrane. However, nanoparticles with bumpy surfaces (curvature diameter of bumps as that of particles <22 nm) were only partially enveloped by the lipid bilayer. For the range of nanostructure dimensions between 1.2 and 22 nm, the lipid membrane underwent structural rearrangements by forming pores (holes). The nanoparticles were accommodated into the pores but not enveloped by the lipid bilayer. The study also found that the lipid membrane conformed to the substrate with surface structures of dimensions less than 1.2 nm without losing the membrane integrity. The experimental results are in accord with the analytical free energy model, which describes the membrane coverage, and numerical simulations which evaluate adhesion of the membrane and dynamics as a function of surface topology. The results obtained in this study are useful for the selection of dimensions and shapes for drug-delivery cargo and for the substrate for supported lipid bilayers. They also help in qualitative understanding the role of length scales involved in the mechanisms of endocytosis and cytotoxicity of nanoparticles. These findings provide a new approach for patterning supported lipid membranes with well-defined features in the 1.2-22 nm range.

摘要

在原子力显微镜实验中,发现了磷脂(二肉豆蔻酰磷脂酰胆碱,DMPC)膜形态在纳米结构二氧化硅表面附近的微小细节。在实验中,通过将不同直径的二氧化硅纳米颗粒沉积在平面光滑的二氧化硅基底上,改变了二氧化硅表面的结构特征。研究发现,由于脂质膜的屏障作用,只有直径大于22 nm且表面光滑的颗粒才会被脂质膜完全包裹。然而,表面有凸起的纳米颗粒(凸起的曲率直径与直径小于22 nm的颗粒相同)仅被脂质双分子层部分包裹。对于纳米结构尺寸在1.2至22 nm之间的范围,脂质膜通过形成孔隙(孔洞)进行结构重排。纳米颗粒被容纳在孔隙中,但未被脂质双分子层包裹。该研究还发现,脂质膜能够贴合尺寸小于1.2 nm的具有表面结构的基底,且不会失去膜的完整性。实验结果与描述膜覆盖率的解析自由能模型以及评估膜的附着力和动力学作为表面拓扑函数的数值模拟结果一致。本研究所得结果对于选择药物递送载体的尺寸和形状以及支撑脂质双分子层的基底具有重要意义。它们还有助于定性理解纳米颗粒内吞作用和细胞毒性机制中涉及的长度尺度的作用。这些发现为在1.2 - 22 nm范围内构建具有明确特征的支撑脂质膜提供了一种新方法。

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