Molecular Mechanisms behind the Anti Corona Virus Activity of Small Metal Oxide Nanoparticles

IF 5.8 3区材料科学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Nanoscale Pub Date : 2025-01-17 DOI:10.1039/d4nr03730h

Björn Greijer, Alexandra Nefedova, Tatiana Agback, Peter Agback, Vambola Kisand, Kai Rausalu, Alexander Vanetsev, Gulaim A. Seisenbaeva, Angela Ivask, Vadim G Kessler

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Abstract

Recent COVID-19 pandemic has set strong quest for advanced understanding of possible tracks in abating and eliminating viral infections. In the view that several families of “pristine” small oxide nanoparticles (NPs) have demonstrated virucidal activity against SARS-CoV-2, we studied the effect of two NPs with presumably different reactivity, on two viruses aiming to evaluate two “primary suspect” routes of their antiviral activity, either specific blocking of surface proteins or causing membrane disruption. The chosen NPs were non-photoactive 3.5 nm triethanolamine terminated (surface capped) titania TiO2 NPs (TATT) and ultrasmall (1.1 nm) silicotungstate polyoxometalate (POM) NPs. The former were expected to both, interact with viral surface proteins as well as strongly complex with phosphate groups whereas the latter was not expected to form surface complexes. We demonstrated that expectedly, POM NPs up to 1.25 mM (4.5 mg/l) had no significant antiviral activity towards neither of the used viruses, an enveloped transmissible gastroenteritis virus (TGEV) belonging to coronaviruses and non-enveloped encelomyocarditis virus (EMCV). At the same time, TATT NPs exhibited statistically significant (p<0.05) antiviral activity against TGEV starting from 0.125 mM (12 µg/ml). However, no antiviral activity of TATT against non-enveloped EMCV was detected. The observation that TATT NPs showed activity only against enveloped viruses and at relatively high concentrations suggests that the effect could be related with complexation with phospholipids. Possible chemical mechanism of viral membrane disruption was investigated by a variable temperature NMR study of NP complexation with model organic phosphate molecules, proving TATT to strongly interact with them and POM remain unreacted. Viral membrane disruption by TATT NPs was additionally confirmed by demonstraing RNA leackage from TGEV upon contact with those NPs. Therefore, our study proved a new mechanism of antiviral action of titania NPs in the dark which involved membrane disruption proceeding via direct surface complexation.

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小金属氧化物纳米颗粒抗冠状病毒活性的分子机制

最近的 COVID-19 大流行使人们强烈要求进一步了解减轻和消除病毒感染的可能途径。有鉴于多个 "原始 "小氧化物纳米粒子（NPs）家族对 SARS-CoV-2 具有杀病毒活性，我们研究了两种可能具有不同反应活性的 NPs 对两种病毒的影响，旨在评估其抗病毒活性的两种 "主要可疑 "途径，即特异性阻断表面蛋白或导致膜破坏。所选的 NPs 是 3.5 nm 三乙醇胺末端（表面封端）非光活性二氧化钛 NPs（TATT）和超小型（1.1 nm）硅钨酸盐聚氧化金属（POM）NPs。预计前者既能与病毒表面蛋白相互作用，又能与磷酸基团形成强烈的复合物，而后者则不会形成表面复合物。我们的研究结果表明，最高达 1.25 毫摩尔（4.5 毫克/升）的 POM NPs 对所使用的两种病毒（属于冠状病毒的有包膜传染性胃肠炎病毒（TGEV）和无包膜心包炎病毒（EMCV））都没有明显的抗病毒活性。同时，从 0.125 mM（12 µg/ml）开始，TATT NPs 对 TGEV 的抗病毒活性具有统计学意义（p<0.05）。但是，没有检测到 TATT 对无包膜 EMCV 的抗病毒活性。TATT NPs 只对有包膜病毒有活性，而且浓度相对较高，这表明其效果可能与磷脂的复合物有关。通过对 NP 与模型有机磷酸盐分子络合的变温核磁共振研究，研究了病毒膜破坏的可能化学机制，结果证明 TATT 与这些分子发生了强烈的相互作用，而 POM 仍未发生反应。此外，TATT NPs 对病毒膜的破坏作用还通过证明 TGEV 在接触这些 NPs 后发生 RNA 泄漏而得到证实。因此，我们的研究证明了二氧化钛纳米粒子在黑暗中抗病毒的新机制，即通过直接的表面复合作用破坏病毒膜。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Nanoscale CHEMISTRY, MULTIDISCIPLINARY-NANOSCIENCE & NANOTECHNOLOGY

CiteScore

12.10

自引率

3.00%

发文量

1628

审稿时长

1.6 months

期刊介绍： Nanoscale is a high-impact international journal, publishing high-quality research across nanoscience and nanotechnology. Nanoscale publishes a full mix of research articles on experimental and theoretical work, including reviews, communications, and full papers.Highly interdisciplinary, this journal appeals to scientists, researchers and professionals interested in nanoscience and nanotechnology, quantum materials and quantum technology, including the areas of physics, chemistry, biology, medicine, materials, energy/environment, information technology, detection science, healthcare and drug discovery, and electronics.