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Study of the functional peptides and peptidolipids in two dimensions: A surface chemistry approach.

机译:在两个方面研究功能性肽和肽脂质:表面化学方法。

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Primarily, this dissertation describes a unique 2D approach that has novel film architecture by controlling a balance of hydrogen-bonding and van der Waals forces. The study suggests that the highly correlated physical parameters are useful to develop new film architecture.; Polymerization of a cysteinyl peptidolipid Langmuir film at the air-water interface is presented. Intermolecular disulfide bonds of the peptidolipid formation of sulfhydryl groups were triggered by oxygen flushed in the water subphase in slightly alkaline condition. The epi-fluorescence and ESEM microscopies were used to study the topography of the polymers formed in either Langmuir or LB films. Increased stability and rigidity of the Langmuir film formed by the cysteinyl peptidolipid could possibly broaden its applications in sensors, biomembranes and other areas.; Next, this dissertation will enrich knowledge of the neuritic plaques formed by amyloid beta peptide (Abeta); Abeta plays a seminal role in the pathogenesis of Alzheimer's disease (AD). Abeta sequence 31--35 (IIGLM) and 25--35 (GSNKGAIIGLM) are among the most frequently studied Abeta derivatives. These fragments possess the structural characteristic of Abeta and retain its neurotoxicity. We apply the two dimensional (2D) approach to investigate the aggregation of these fragments. To improve their stability and self-assembly at the air-water interface, the fragments were modified with an aliphatic chain at the N-terminus of the peptide's carboxylic acid or amide moieties. Surface chemistry techniques were applied to monitor the aggregation process and the real time epi-fluorescence microscopy was utilized to observe the topography of the domains formed, whereas IRRAS provided the information on the spectral features of the domains at the air-water interface. Supplementary spectroscopic techniques including MAIR, RA, CD and ATR-FTIR were used to investigate the conformation of the domains in the LB film. Finally, aggregates formed with Abeta (31--35) and Abeta (1--42) were labeled using luminescent CdSe/ZnS Quantum Dots, this renders a higher intensity and better contrast for imaging the aggregates. This study aims to assist in the elucidation of the aggregation mechanism, potentially aiding the discovery of an effective cure for AD.
机译:首先,本文描述了一种独特的2D方法,该方法通过控制氢键和范德华力的平衡而具有新颖的薄膜结构。研究表明,高度相关的物理参数对于开发新的胶片结构很有用。半胱氨酰肽脂Langmuir膜在空气-水界面的聚合反应。巯基基团的肽脂质形成的分子间二硫键由在弱碱性条件下在水亚相中冲洗的氧气触发。落射荧光和ESEM显微镜用于研究在Langmuir或LB膜中形成的聚合物的形貌。半胱氨酰肽脂质形成的Langmuir膜的稳定性和刚性的提高可能会扩大其在传感器,生物膜和其他领域的应用。接下来,本论文将丰富对淀粉样β肽(Abeta)形成的神经斑的知识。 Abeta在阿尔茨海默氏病(AD)的发病机理中起着重要作用。 Abeta序列31--35(IIGLM)和25--35(GSNKGAIIGLM)是最常研究的Abeta衍生物。这些片段具有Abeta的结构特征,并保留其神经毒性。我们应用二维(2D)方法来研究这些片段的聚集。为了提高它们在空气-水界面的稳定性和自组装性,将片段在肽的羧酸或酰胺部分的N端用脂族链修饰。应用表面化学技术监测聚集过程,并利用实时落射荧光显微镜观察形成的畴的形貌,而IRRAS提供了有关气-水界面上畴的光谱特征的信息。辅助光谱技术包括MAIR,RA,CD和ATR-FTIR用于研究LB膜中结构域的构象。最后,使用发光的CdSe / ZnS量子点标记由Abeta(31--35)和Abeta(1-42)形成的聚集体,这为聚集体成像提供了更高的强度和更好的对比度。这项研究旨在协助阐明聚集机制,可能有助于发现有效的AD治疗方法。

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