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Molecular Thermodynamics of Superheated Lipid-Coated Fluorocarbon Nanoemulsions.

机译:过热脂质包覆的氟碳纳米乳液的分子热力学。

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摘要

Diagnostic ultrasound is a safe, inexpensive and highly portable real-time imaging modality for viewing the human body. For over two decades, lipid-coated fluorocarbon microbubble contrast agents have been developed to help improve the diagnostic and therapeutic capabilities of ultrasound, but they have certain limitations. Recently, it was found that the microbubbles can be condensed into superheated liquid nanodrops capable of being vaporized by external optical or acoustic triggers. The compact form and vaporization effects of these phase-shift nanodrops may offer advantages over microbubbles for a number of current and future therapeutic and diagnostic applications. The goal of this dissertation work was to study the molecular thermodynamics and interfacial phenomena of these superheated phase-shift nanodrops.;In the first part of this work, a custom microscopy pressure chamber with control over temperature and pressure was used to observe microbubbles during condensation. Compression behaviors of fluorocarbon microbubbles constructed with lipid shells of varying acyl chain lengths were quantified over a broad temperature range. Microbubbles containing lipids of longer acyl chains were found to resist ideal compression and condensation. Dissolution was found to dominate as temperature approached the lipid main phase transition temperature, resulting in incomplete condensation. However, successful condensation of gas-filled microbubbles to liquid-filled nanodrops could be achieved at lower temperatures, and fluorescence microscopy showed that the lipid monolayer shell buckles and folds into surface-attached bilayer strands. The nanodrops were found to be remarkably stable when brought back to standard temperature and pressure. The temperature-pressure data were used to construct condensation phase diagrams to determine the thresholds for successful nanodrop formation.;In the second part of this study, the superheated nanodrops were vaporized back into microbubbles by changes in temperature and pressure. A custom optical chamber with control over temperature and pressure was used to track the kinetics of condensation, vaporization and dissolution of microbubble suspensions with varying fluorocarbon core and lipid shell compositions. A simple model was used to extract kinetic rates from the optical data, and Arrhenius plots were used to determine activation energies. The activation energy for thermal vaporization was found to vary with lipid acyl chain length, and a simple model of lipid intermolecular forces was used to explain this effect. Additionally, thermal vaporization was found to occur near 90% of the critical temperature of the fluorocarbon core, indicating that metastability of the superheated droplets was due to the low probability of homogenous nucleation rather than a Laplace overpressure. The superheated droplets could be reversibly vaporized and condensed to at least ten cycles, showing remarkable stability.;In the final part of this study, the tunability of vaporization was examined through the mixing of fluorocarbon gases in droplet core. A clinical ultrasound imaging system was used to track vaporization as a function of temperature and mechanical index. Discrepancies were found in the vaporization thresholds owing to mass transfer; the high solubility of the lower fluorocarbon caused it to rapidly deplete. However, a successful acoustic temperature probe was demonstrated. The experimental data from all three parts of this study were examined and explained by conventional molecular thermodynamics theory, providing new insights into the behavior and properties of these novel theranostic agents.
机译:诊断超声是用于查看人体的安全,廉价且高度便携的实时成像方式。二十多年来,已开发出脂质包裹的碳氟化合物微泡造影剂,以帮助改善超声的诊断和治疗能力,但它们具有一定的局限性。最近,发现微泡可被冷凝成能够被外部光学或声学触发物汽化的过热液体纳米滴。对于许多当前和未来的治疗和诊断应用,这些相移纳米滴的紧凑形式和汽化效果可能提供优于微泡的优势。本论文的目的是研究这些过热的相移纳米液滴的分子热力学和界面现象。在这项工作的第一部分中,使用定制的显微镜压力室来控制温度和压力,以观察冷凝过程中的微气泡。 。在广泛的温度范围内,量化了具有不同酰基链长度的脂质壳构成的碳氟化合物微气泡的压缩行为。发现含有更长酰基链的脂质的微泡可抵抗理想的压缩和缩合。发现当温度接近脂质主相转变温度时,溶解占主导,导致不完全缩合。然而,可以在较低的温度下将充气微泡成功凝结成液体纳米滴,荧光显微镜显示脂质单层壳弯曲并折叠成表面附着的双层链。发现当回到标准温度和压力时,纳米滴是非常稳定的。温度-压力数据用于构建冷凝相图,以确定成功形成纳米滴的阈值。在本研究的第二部分中,由于温度和压力的变化,过热的纳米滴被汽化回微气泡。使用可控制温度和压力的定制光学室来跟踪具有变化的碳氟化合物核和脂质壳成分的微泡悬浮液的冷凝,汽化和溶解动力学。使用一个简单的模型从光学数据中提取动力学速率,并使用Arrhenius曲线确定活化能。发现用于热汽化的活化能随脂质酰基链的长度而变化,并且使用脂质分子间力的简单模型来解释该作用。另外,发现热蒸发发生在碳氟化合物核的临界温度的接近90%处,这表明过热的液滴的亚稳态是由于均匀成核的可能性较低,而不是由于拉普拉斯过压所致。过热的液滴可以可逆地汽化并冷凝至至少十个循环,显示出显着的稳定性。在本研究的最后部分,通过碳氟化合物气体在液滴芯中的混合来检验汽化的可调性。临床超声成像系统用于跟踪汽化温度和机械指数的函数。由于传质,在汽化阈值中发现差异。低级碳氟化合物的高溶解度使其迅速耗尽。然而,证明了成功的声温探测器。通过常规分子热力学理论对本研究的所有三个部分的实验数据进行了检查和解释,为这些新型治疗剂的行为和性质提供了新的见解。

著录项

  • 作者

    Mountford, Paul A. C.;

  • 作者单位

    University of Colorado at Boulder.;

  • 授予单位 University of Colorado at Boulder.;
  • 学科 Biomedical engineering.
  • 学位 Ph.D.
  • 年度 2015
  • 页码 191 p.
  • 总页数 191
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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