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Characterization of novel molecular photoacoustic contrast agents for in vivo photoacoustic tomography.

机译:用于体内光声层析成像的新型分子光声造影剂的表征。

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摘要

Photoacoustic tomography is a hybrid imaging modality that takes advantage of the high contrast of pure optical imaging and the high intrinsic resolution of ultrasound without the necessity of ionizing radiation. Photoacoustic imaging (PM) is neither purely optical nor purely acoustical in nature, but a combination of the two. It is fundamentally based on light excitation and ultrasonic detection. Photoacoustic imaging has been successful without the introduction of exogenous contrast agents; however, to image deeper regions of biological tissue, a contrast agent is necessary. Several types of photoacoustic contrast agents have been made available for diagnostic purposes; however, the majority of literature has focused on gold nanoparticle systems for which the surface-plasmon resonance effect is important. The only option currently available for molecular PM contrast agents is to choose an existing near infrared absorbing fluorescent probes with the hope that they may generate a substantial photoacoustic (PA) response. However, these dyes have been designed with an optimized fluorescence emission response and are not anticipated to generate an adequate photoacoustic response. This dissertation addresses this lack of precedence in the literature for understanding the mechanism of a photoacoustic signal generation from strongly absorbing dye molecules including BODIPY, cyanine and curcumin systems. This work represents preliminary efforts in bringing novel molecular photoacoustic contrast agents (MPACs) into the photoacoustic imaging arena. To this end, photoacoustic and optical Z-scan experiments, and quenching studies were employed to demonstrate correlation of photoacoustic emission enhancement with excited state absorption mechanisms. To investigate further the photoacoustic emission in a practical imaging setting, MPACs were imaged using a recently developed photoacoustic imaging tomography system which was constructed exclusively for the purpose of this study.
机译:光声层析成像是一种混合成像方式,它利用了纯光学成像的高对比度和超声的高固有分辨率,而无需电离辐射。光声成像(PM)本质上既不是纯光学的也不是纯声学的,而是两者的结合。它从根本上基于光激发和超声波检测。没有引入外源性造影剂,光声成像是成功的。但是,要使生物组织的较深区域成像,必须使用造影剂。为了诊断目的,已经提供了几种类型的光声对比剂。然而,大多数文献集中在金纳米粒子系统上,表面等离子共振效应是重要的。分子PM造影剂当前唯一可用的选择是选择现有的近红外吸收荧光探针,希望它们可以产生大量的光声(PA)响应。然而,这些染料被设计为具有优化的荧光发射响应,并且预期不会产生足够的光声响应。本论文解决了文献中缺乏先验知识的问题,该文献缺乏理解从包括BODIPY,花青和姜黄素系统的强吸收染料分子产生光声信号的机理。这项工作代表了将新型分子光声造影剂(MPAC)引入光声成像领域的初步努力。为此,采用了光声和光学Z扫描实验以及淬灭研究来证明光声发射增强与激发态吸收机理之间的相关性。为了进一步研究在实际成像环境中的光声发射,使用最近开发的光声成像层析成像系统对MPAC成像,该系统是专门为本研究目的而构建的。

著录项

  • 作者

    Laoui, Samir.;

  • 作者单位

    University of Massachusetts Lowell.;

  • 授予单位 University of Massachusetts Lowell.;
  • 学科 Physics.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 88 p.
  • 总页数 88
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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