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Identification of Biomolecular Building Blocks by Recognition Tunneling: Stride towards Nanopore Sequencing of Biomolecules.

机译:通过识别隧道识别生物分子构件:迈向生物分子的纳米孔测序。

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摘要

DNA, RNA and Protein are three pivotal biomolecules in human and other organisms, playing decisive roles in functionality, appearance, diseases development and other physiological phenomena. Hence, sequencing of these biomolecules acquires the prime interest in the scientific community. Single molecular identification of their building blocks can be done by a technique called Recognition Tunneling (RT) based on Scanning Tunneling Microscope (STM). A single layer of specially designed recognition molecule is attached to the STM electrodes, which trap the targeted molecules (DNA nucleoside monophosphates, RNA nucleoside monophosphates or amino acids) inside the STM nanogap. Depending on their different binding interactions with the recognition molecules, the analyte molecules generate stochastic signal trains accommodating their "electronic fingerprints". Signal features are used to detect the molecules using a machine learning algorithm and different molecules can be identified with significantly high accuracy. This, in turn, paves the way for rapid, economical nanopore sequencing platform, overcoming the drawbacks of Next Generation Sequencing (NGS) techniques.;To read DNA nucleotides with high accuracy in an STM tunnel junction a series of nitrogen-based heterocycles were designed and examined to check their capabilities to interact with naturally occurring DNA nucleotides by hydrogen bonding in the tunnel junction. These recognition molecules are Benzimidazole, Imidazole, Triazole and Pyrrole. Benzimidazole proved to be best among them showing DNA nucleotide classification accuracy close to 99%. Also, Imidazole reader can read an abasic monophosphate (AP), a product from depurination or depyrimidination that occurs 10,000 times per human cell per day.;In another study, I have investigated a new universal reader, 1-(2-mercaptoethyl)pyrene (Pyrene reader) based on stacking interactions, which should be more specific to the canonical DNA nucleosides. In addition, Pyrene reader showed higher DNA base-calling accuracy compare to Imidazole reader, the workhorse in our previous projects. In my other projects, various amino acids and RNA nucleoside monophosphates were also classified with significantly high accuracy using RT. Twenty naturally occurring amino acids and various RNA nucleosides (four canonical and two modified) were successfully identified. Thus, we envision nanopore sequencing biomolecules using Recognition Tunneling (RT) that should provide comprehensive betterment over current technologies in terms of time, chemical and instrumental cost and capability of de novo sequencing.
机译:DNA,RNA和蛋白质是人类和其他生物中的三个关键生物分子,在功能,外观,疾病发展和其他生理现象中起着决定性的作用。因此,这些生物分子的测序引起了科学界的主要兴趣。可以通过基于扫描隧道显微镜(STM)的称为识别隧道(RT)的技术对它们的结构单元进行单分子鉴定。单层经过特殊设计的识别分子附着在STM电极上,该电极将目标分子(DNA核苷单磷酸,RNA核苷单磷酸或氨基酸)捕获在STM纳米间隙内。根据它们与识别分子的不同结合相互作用,分析物分子产生容纳其“电子指纹”的随机信号链。信号特征用于使用机器学习算法检测分子,并且可以以非常高的准确性识别不同的分子。反过来,这为快速,经济的纳米孔测序平台铺平了道路,克服了下一代测序(NGS)技术的缺点。为了在STM隧道连接中高精度读取DNA核苷酸,设计了一系列基于氮的杂环并检查了它们通过隧道结中的氢键与天然存在的DNA核苷酸相互作用的能力。这些识别分子是苯并咪唑,咪唑,三唑和吡咯。苯并咪唑被证明是最好的,显示出DNA核苷酸分类准确率接近99%。同样,咪唑阅读器可以读取脱碱基或去嘧啶化的无碱基一磷酸(AP),每个人细胞每天发生10,000次。;在另一项研究中,我研究了一种新型通用读取器1-(2-巯基乙基)py (P阅读器)基于堆积的相互作用,这应该对规范的DNA核苷更具特异性。此外,与我们以前项目中的主力咪唑阅读器相比,P阅读器显示出更高的DNA碱基调用准确性。在我的其他项目中,还使用RT对各种氨基酸和RNA核苷一磷酸进行了非常高的分类。已成功鉴定出20种天然氨基酸和各种RNA核苷(4个规范氨基酸和2个修饰氨基酸)。因此,我们设想使用识别隧道(RT)的纳米孔测序生物分子,它在时间,化学和仪器成本以及从头测序的能力方面应比当前技术提供全面的改进。

著录项

  • 作者

    Sen, Suman.;

  • 作者单位

    Arizona State University.;

  • 授予单位 Arizona State University.;
  • 学科 Nanoscience.;Biophysics.
  • 学位 Ph.D.
  • 年度 2016
  • 页码 148 p.
  • 总页数 148
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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