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通过细胞膜中的载体研究 siRNA 介导的输送中的离子条件:分子动力学模拟。

Investigation of the ionic conditions in SiRNA-mediated delivery through its carriers in the cell membrane: a molecular dynamic simulation.

机构信息

Nanobiotechnology Research Center, Baqiyatallah University of Medical Sciences, Tehran, Iran.

Department of Biophysics, Faculty of Biological Science, Tarbiat Modares University, Tehran, 14115-154, Iran.

出版信息

Sci Rep. 2022 Oct 20;12(1):17520. doi: 10.1038/s41598-022-22509-1.

Abstract

SiRNA is a new generation of drug molecules and a new approach for treating a variety of diseases such as cancer and viral infections. SiRNA delivery to cells and translocation into cytoplasm are the main challenges in the clinical application of siRNA. Lipid carriers are one of the most successful carriers for siRNA delivery. In this study, we investigated the interaction of siRNA with a zwitterionic bilayer and how ion concentration and lipid conjugation can affect it. The divalent cation such as Mg ions could promote the siRNA adsorption on the bilayer surface. The cation ions can bind to the head groups of lipids and the grooves of siRNA molecules and form bridges between the siRNA and bilayer surface. Our findings demonstrated the bridges formed by divalent ions could facilitate the attachment of siRNA to the membrane surface. We showed that the divalent cations can regulate the bridging-driven membrane attachment and it seems the result of this modulation can be used for designing biomimetic devices. In the following, we examined the effect of cations on the interaction between siRNA modified by cholesterol and the membrane surface. Our MD simulations showed that in the presence of Mg, the electrostatic and vdW energy between the membrane and siRNA were higher compared to those in the presence of NA. We showed that the electrostatic interaction between membrane and siRNA cannot be facilitated only by cholesterol conjugated. Indeed, cations are essential to create coulomb repulsion and enable membrane attachment. This study provides important insight into liposome carriers for siRNA delivery and could help us in the development of siRNA-based therapeutics. Due to the coronavirus pandemic outbreak, these results may shed light on the new approach for treating these diseases and their molecular details.

摘要

siRNA 是新一代的药物分子,是治疗癌症和病毒感染等多种疾病的新方法。将 siRNA 递送到细胞并转位到细胞质是 siRNA 临床应用的主要挑战。脂质载体是 siRNA 递送的最成功载体之一。在这项研究中,我们研究了 siRNA 与两性离子双层的相互作用,以及离子浓度和脂质缀合如何影响这种相互作用。二价阳离子(如 Mg 离子)可以促进 siRNA 在双层表面的吸附。阳离子可以结合到脂质的头基和 siRNA 分子的沟槽中,并在 siRNA 和双层表面之间形成桥。我们的发现表明,二价离子形成的桥可以促进 siRNA 与膜表面的附着。我们表明,二价阳离子可以调节桥接驱动的膜附着,这种调节的结果似乎可以用于设计仿生装置。在接下来的研究中,我们研究了阳离子对胆固醇修饰的 siRNA 与膜表面相互作用的影响。我们的 MD 模拟表明,在存在 Mg 的情况下,与存在 Na 相比,膜和 siRNA 之间的静电和 vdW 能更高。我们表明,仅通过胆固醇修饰不能促进膜和 siRNA 之间的静电相互作用。事实上,阳离子对于产生库仑排斥并使膜附着是必不可少的。这项研究为 siRNA 递送至脂质体载体提供了重要的见解,并可能有助于我们开发基于 siRNA 的治疗方法。由于冠状病毒大流行的爆发,这些结果可能为治疗这些疾病及其分子细节提供新的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/55ed/9584942/7d06fc43ff2a/41598_2022_22509_Fig1_HTML.jpg

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