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Mesoporous silica nanomaterials for applications in catalysis, sensing, drug delivery and gene transfection

机译:介孔二氧化硅纳米材料,用于催化,传感,药物递送和基因转染

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摘要

The central theme of this dissertation is represented by the versatility of mesoporous silica nanomaterials in various applications such as catalysis and bio-applications, with main focus on biological applications of Mesoporous Silica Nanospheres (MSN). The metamorphosis that we impose to these materials from catalysis to sensing and to drug and gene delivery is detailed in this dissertation. First, we developed a synthetic method that can fine tune the amount of chemically accessible organic functional groups on the pores surface of MSN by exploiting electrostatic and size matching between the cationic alkylammonium head group of the CTAB surfactant and various anionic organoalkoxysilane precursors at the micelle-water interface in a base-catalyzed condensation reaction of silicate.;Aiming nature imitation, we demonstrated the catalytic abilities of the MSNs. We utilized an ethylenediamine functional group for chelating Cu 2+ as a catalytic functional group anchored inside the mesopores. Thus, a polyalkynylene-based conducting polymer (molecular wire) was synthesized within the Cu-functionalized MSNs silica catalyst.;For sensing applications, we have synthesized a poly(lactic acid) coated mesoporous silica nanosphere (PLA-MSN) material that serves as a fluorescence sensor system for detection of amino-containing neurotransmitters in neutral aqueous buffer. We exploited the mesoporosity of MSNs for encapsulating pharmaceutical drugs. We examined bio-friendly capping molecules such as polyamidoamine dendrimers of generations G2 to G4, to prevent the drug leaching. Next, the drug delivery system employed MSNs loaded with Doxorubicin, an anticancer drug. The results demonstrated that these nano-Trojan horses have ability to deliver Doxorubicin to cancer cells and induce their death.;Finally, to demonstrate the potential of MSN as an universal cellular transmembrane nanovehicle, we anchored positively charged dendrimers on the surface of MSN and utilize them to complex cationic DNA. The p-EGFP-C1 gene-coated MSN nanocomposite was able to transfect cancer cell lines, such as human HeLa and CHO cancer cell lines. The gene carrier ability of MSNs was further proved by transfecting primary cells and cotransfecting of two different genes in cancer cell lines.;In sum, MSN are versatile partners in several types of applications, as demonstrated in the 164 pages of my dissertation.
机译:本文的中心主题是介孔二氧化硅纳米材料在催化和生物应用等各种应用中的多功能性,主要关注介孔二氧化硅纳米球的生物应用。本文详细介绍了我们从催化到传感,再到药物和基因传递所赋予的这些变态。首先,我们开发了一种合成方法,可以利用CTAB表面活性剂的阳离子烷基铵头基与胶束中各种阴离子有机烷氧基硅烷前体之间的静电和大小匹配,来微调MSN孔表面上化学可及的有机官能团的数量。碱催化的硅酸盐缩合反应中的水界面。针对自然模拟,我们证明了MSNs的催化能力。我们利用乙二胺官能团螯合Cu 2+作为锚定在中孔内的催化官能团。因此,在Cu功能化的MSNs二氧化硅催化剂中合成了基于聚亚炔基的导电聚合物(分子线).;对于传感应用,我们已经合成了涂覆有聚乳酸的介孔二氧化硅纳米球(PLA-MSN)材料,荧光传感器系统,用于检测中性水性缓冲液中的含氨基神经递质。我们利用MSN的介孔性来封装药物。我们检查了生物友好的加帽分子,例如G2至G4代的聚酰胺酰胺树状聚合物,以防止药物浸出。接下来,药物输送系统采用装有抗癌药阿霉素的MSN。结果表明,这些纳米特洛伊木马具有将阿霉素递送至癌细胞并诱导其死亡的能力。最后,为了证明MSN作为通用细胞跨膜纳米载体的潜力,我们将带正电的树状分子锚定在MSN表面并利用它们形成复杂的阳离子DNA。涂有p-EGFP-C1基因的MSN纳米复合材料能够转染癌细胞系,例如人HeLa和CHO癌细胞系。通过转染原代细胞并共同转染癌细胞系中两个不同的基因,进一步证明了MSNs的基因携带能力。总之,如本文164页所述,MSN在多种类型的应用中是通用伙伴。

著录项

  • 作者

    Radu, Daniela Rodica;

  • 作者单位
  • 年度 2004
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  • 原文格式 PDF
  • 正文语种 en
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