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The Synthesis of N-Acetyllactosamine Functionalized Dendrimers, and the Functionalization of Silica Surfaces Using Tunable Dendrons and beta-Cyclodextrins

机译:N-乙酰乙酰氨基胺官能化的树枝状大分子的合成,以及使用可调式树枝和β-环糊精对二氧化硅表面的官能化

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摘要

Galectin-3 is beta-galactoside binding protein which is found in many healthy cells. In cancer, the galectin-3/tumor-associated Thomsen-Friedenreich antigen (TF antigen) interaction has been implicated in heterotypic and homotypic cellular adhesion and apoptotic signaling pathways. However, a stronger mechanistic understanding of the role of galectin-3 in these processes is needed. N-acetyllactosamine (LacNAc) is a non-native ligand for galectin-3 which binds with comparable affinity to the TF antigen and therefore an important ligand to study galectin-3 mediated processes.;To study galectin-3 mediated homotypic cellular aggregation, four generations of polyamidoamine (PAMAM) dendrimers were functionalized with N-acetyllactosamine using a four-step chemoenzymatic route. The enzymatic step controlled the regiochemistry of the galactose addition to N-acetylglucosamine functionalized dendrimers using a recombinant beta-1,4-Galactosyltransferase-/UDP-4'-Gal Epimerase Fusion Protein (lgtB-galE). Homotypic cellular aggregation, which is promoted by the presence of galectin-3 as it binds to glycosides at the cell surface, was studied using HT-1080 fibrosarcoma, A549 lung, and DU-145 prostate cancer cell lines. In the presence of small LacNAc functionalized PAMAM dendrimers, galectin-3 induced cancer cellular aggregation was inhibited. However, the larger glycodendrimers induced homotypic cellular aggregation.;Additionally, novel poly(aryl ether) dendronized silica surfaces designed for reversible adsorbtion of targeted analytes were synthesized, and characterization using X-ray Photoelectron Spectroscopy (XPS) was performed. Using a Cu(I) mediated cycloaddition "click" reaction, beta-cyclodextrin was appended to dendronized surfaces via triazole formation and also to a non-dendronized surface for comparison purposes. First generation G(1) dendrons have more than 6 times greater capacity to adsorb targeted analytes than slides functionalized with monomeric beta-cyclodextrin and are 2 times greater than slides functionalized with larger generation dendrons. This study reported beta-cyclodextrin functionalized surfaces can undergo a triggered release of the adsorbent, but otherwise retained the targeted analyte through multiple aqueous washes. Therefore, a new generation of G(1) dendronized surfaces capable of reversible adsorption were developed by heterogeneously appending sulfonic acid/pyridine end-groups. Auger Electron Spectroscopy (AES) was used to quantify the ratio of groups installed. Furthermore, G(1) dendronized surfaces were functionalized homogenously with sulfonic acid and pyridine for comparison and with chiral amino acids for chiral recognition studies.
机译:Galectin-3是在许多健康细胞中发现的β-半乳糖苷结合蛋白。在癌症中,galectin-3 /肿瘤相关的Thomsen-Friedenreich抗原(TF抗原)相互作用涉及异型和同型细胞粘附和凋亡信号通路。但是,需要对半乳凝素3在这些过程中的作用有更强的机理理解。 N-乙酰基乳糖胺(LacNAc)是Galectin-3的非天然配体,与TF抗原具有相当的亲和力,因此是研究galectin-3介导的过程的重要配体。研究galectin-3介导的同型细胞聚集,四个N-乙酰基乳糖胺通过四步化学酶法途径将多代聚酰胺酰胺(PAMAM)树状聚合物官能化。酶促步骤控制了使用重组β-1,4-半乳糖基转移酶-/ UDP-4'-Gal Epimerase融合蛋白(lgtB-galE)将半乳糖添加到N-乙酰氨基葡糖官能化树状聚合物中的区域化学作用。使用HT-1080纤维肉瘤,A549肺和DU-145前列腺癌细胞系研究了半乳糖凝集素3的存在促进的同型细胞聚集,因为它与细胞表面的糖苷结合。在小的LacNAc功能化PAMAM树状聚合物的存在下,galectin-3诱导的癌细胞聚集受到抑制。然而,较大的糖类树状聚合物诱导了同型细胞聚集。此外,合成了设计用于目标分析物可逆吸附的新型聚(芳醚)树枝状二氧化硅表面,并使用X射线光电子能谱(XPS)进行了表征。使用Cu(I)介导的环加成“点击”反应,将β-环糊精通过三唑形成附接到树枝化表面上,并且为了比较目的还附加到未树枝化表面上。第一代G(1)树突的吸附目标分析物的能力是用单体β-环糊精功能化的载玻片的6倍以上,并且是使用较大世代树突功能化的玻片的2倍以上。这项研究报告称,β-环糊精官能化的表面可经历吸附剂的触发释放,但通过多次水洗保留了目标分析物。因此,通过异质性地附加磺酸/吡啶端基,开发了一种具有可逆吸附能力的新一代G(1)树状表面。俄歇电子能谱(AES)用于量化已安装组的比率。此外,G(1)树突化的表面用磺酸和吡啶进行均质化以进行比较,并用手性氨基酸进行手性识别研究。

著录项

  • 作者

    Ennist, Jessica Helen.;

  • 作者单位

    Montana State University.;

  • 授予单位 Montana State University.;
  • 学科 Organic chemistry.
  • 学位 Ph.D.
  • 年度 2017
  • 页码 292 p.
  • 总页数 292
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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