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Specific Amino Acid Substitutions Improve the Activity and Specificity of an Antimicrobial Peptide & Serodiagnosis by Immunosignature: a Multiplexing Tool for Monitoring the Humoral Immune Response to Dengue.

机译:特定氨基酸取代可提高抗菌肽的活性和特异性,并通过免疫签名进行血清诊断:一种用于监测对登革热的体液免疫反应的多路复用工具。

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摘要

Random peptide microarrays are a powerful tool for both the treatment and diagnostics of infectious diseases. On the treatment side, selected random peptides on the microarray have either binding or lytic potency against certain pathogens cells, thus they can be synthesized into new antimicrobial agents, denoted as synbodies (synthetic antibodies). On the diagnostic side, serum containing specific infection-related antibodies create unique and distinct "pathogen-immunosignatures" on the random peptide microarray distinct from the healthy control serum, and this different mode of binding can be used as a more precise measurement than traditional ELISA tests. My thesis project is separated into these two parts: the first part falls into the treatment side and the second one focuses on the diagnostic side.;My first chapter shows that a substitution amino acid peptide library helps to improve the activity of a recently reported synthetic antimicrobial peptide selected by the random peptide microarray. By substituting one or two amino acids of the original lead peptide, the new substitutes show changed hemolytic effects against mouse red blood cells and changed potency against two pathogens: Staphylococcus aureus and Pseudomonas aeruginosa. Two new substitutes are then combined together to form the synbody, which shows a significantly antimicrobial potency against Staphylococcus aureus (<0.5uM).;In the second chapter, I explore the possibility of using the 10K Ver.2 random peptide microarray to monitor the humoral immune response of dengue. Over 2.5 billion people (40% of the world's population) live in dengue transmitting areas. However, currently there is no efficient dengue treatment or vaccine. Here, with limited dengue patient serum samples, we show that the immunosignature has the potential to not only distinguish the dengue infection from non-infected people, but also the primary dengue infection from the secondary dengue infections, dengue infection from West Nile Virus (WNV) infection, and even between different dengue serotypes. By further bioinformatic analysis, we demonstrate that the significant peptides selected to distinguish dengue infected and normal samples may indicate the epitopes responsible for the immune response.
机译:随机肽微阵列是用于治疗和诊断感染性疾病的强大工具。在治疗方面,微阵列上选定的随机肽对某些病原体细胞具有结合力或溶解力,因此可以将它们合成为新的抗菌剂,称为合成抗体(合成抗体)。在诊断方面,含有特异性感染相关抗体的血清会在随机肽微阵列上产生与健康对照血清不同的独特且独特的“病原体免疫签名”,这种不同的结合方式可比传统的ELISA进行更精确的测量测试。我的论文计划分为两个部分:第一部分属于治疗方面,第二部分侧重于诊断方面。;我的第一章表明,取代氨基酸肽库有助于提高最近报道的合成蛋白的活性由随机肽微阵列选择的抗菌肽。通过替代原始先导肽的一个或两个氨基酸,新的替代品显示出对小鼠红细胞的溶血作用发生了变化,并且对两种病原体:金黄色葡萄球菌和铜绿假单胞菌的效力发生了变化。然后将两个新的替代物组合在一起以形成合体,该合体显示出对金黄色葡萄球菌(<0.5uM)显着的抗菌效力。在第二章中,我探讨了使用10K Ver.2随机肽微阵列监测药物的可能性。登革热的体液免疫反应。登革热传播地区生活着超过25亿人(占世界人口的40%)。但是,目前尚无有效的登革热治疗或疫苗。在这里,通过有限的登革热患者血清样本,我们表明免疫印记不仅可以将登革热感染与未感染人群区分开,而且还可以将原发登革热感染与继发登革热感染,西尼罗河病毒(WNV) )感染,甚至在不同的登革热血清型之间。通过进一步的生物信息学分析,我们证明选择用来区分登革热感染和正常样品的重要肽可能表明负责免疫反应的表位。

著录项

  • 作者

    Wang, Xiao.;

  • 作者单位

    Arizona State University.;

  • 授予单位 Arizona State University.;
  • 学科 Biology General.;Biology Microbiology.;Biology Bioinformatics.
  • 学位 M.S.
  • 年度 2013
  • 页码 99 p.
  • 总页数 99
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-17 11:41:11

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