首页> 外文会议>Society for Biomaterials annual meeting and exposition >Lipid-Coated Mesoporous Silica Nanoparticles for Antiviral Delivery to Inhibit Encephalitic Alphavirus Infection
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Lipid-Coated Mesoporous Silica Nanoparticles for Antiviral Delivery to Inhibit Encephalitic Alphavirus Infection

机译:脂质涂覆的介孔二氧化硅纳米粒子的抗病毒传递抑制脑性甲病毒的感染。

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In this work, we highlight the use ot an LC-MSNs technology for loading and release of antiviral ML336 to inhibit a vaccine strain of the VEEV virus. This technology is particularly versatile, and in the future, we intend to improve controlled release through surface modification of the MSN. In addition, we will functionalize lipids with targeting moieties for cell type-specific delivery. The LC-MSNs are also biocompatible and can have long circulation times, which will allow assessment of ML336-loaded LC-MSNs to inhibit virus in an animal model. As a whole, LC-MSNs have the potential to enable delivery of small molecule antivirals, reducing threats from naturally spreading viruses and bioterrorism. This work was funded by the Defense Threat Reduction Agency (DTRA), project 1002720595.
机译:在这项工作中,我们重点介绍了使用LC-MSNs技术装载和释放抗病毒ML336来抑制VEEV病毒的疫苗株。该技术用途特别广泛,将来,我们打算通过对MSN进行表面修饰来改善控制释放。此外,我们将通过靶向部分功能化脂质,以实现细胞类型特异性递送。 LC-MSN也具有生物相容性,并且循环时间长,这将有助于评估ML336负载的LC-MSN在动物模型中抑制病毒的能力。总体而言,LC-MSN具有释放小分子抗病毒药的潜力,可减少自然传播的病毒和生物恐怖主义的威胁。这项工作由美国国防威胁减少局(DTRA)资助,项目1002720595。

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