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Magnetisation transfer contrast as a quantitative MRI technique for the study of bio-polymer systemsPidwell, Anna Louise January 2001 (has links)
No description available.
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Off-resonance correction for magnetic resonance imaging with spiral trajectoriesNylund, Andreas January 2014 (has links)
The procedure of cardiographic magnetic resonance imaging requires patients to hold their breath for up to twenty seconds, creating an uncomfortable situation for many patients. It is proposed that an acquisition scheme using spiral trajectories is preferable due to their much shorter total scan time; however, spiral trajectories suffer from a blurring effect caused by off-resonance frequencies in the image area. There are several methods for reconstructing images with reduced blur and Conjugate Phase Reconstruction has been chosen as a method for implementation into Matlab-script for evaluation in regards to image reconstruction quality and computation time. This method finds a conjugate to the off-resonance from a field map to demodulate the image and an algorithm for frequency‑segmented Conjugate Phase Reconstruction is implemented along with an improvement called Multi-frequency Interpolation. The implementation is tested through simulation of spiral magnetic resonance imaging using a Shepp‑Logan phantom. Different off-resonance frequencies and field maps are used to provide a broad view of the functionality of the code. The two algorithms are then compared to each other in terms of computation speed and image quality. It is concluded that this implementation might reconstruct images well but that further testing on actual scan sequences is required to determine the usefulness. The Multi-frequency Interpolation algorithm yields images that are not useful in a clinical context. Further study of other methods not requiring a field map is suggested for comparison.
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Magnetic Resonance Molecular Imaging Using Iron Oxide NanoparticlesZurkiya, Omar 13 November 2006 (has links)
Magnetic resonance imaging (MRI) is regularly used to obtain anatomical images, greatly advancing biomedical research and clinical health care today, but its full potential in providing functional, physiological, and molecular information is only beginning to emerge. The goal of magnetic resonance molecular imaging is to utilize MRI to acquire information on the molecular level. This dissertation is focused on ways to increase the use of MRI for molecular imaging using superparamagnetic iron oxide (SPIO) nanoparticle induced MRI contrast. This work is divided into three main sections: <B>1)<I> Elucidation of the contribution of size and coating properties to magnetic nanoparticle induced proton relaxation.</I></B> To maximize contrast generated without increasing particle size, new methods to increase effects on relaxivity must be developed. Experimental data obtained on a new class of biocompatible particles are presented, along with simulated data. The effects of coating size, proton exchange, and altered diffusion are examined. Simulations are presented confirming the effect of particle coatings on clustering-induced relaxivity changes, and an experimental system demonstrating the clustering effect is presented. <B>2)<I> Development of a diffusion-dependent, off-resonance imaging protocol for magnetic nanoparticles.</I></B> This work demonstrates an alternative approach, off-resonance saturation (ORS), for generating contrast sensitive to SPIO nanoparticles. This method leads to a calculated contrast that increases with SPIO concentration. Experimental data and a mathematical model demonstrate and characterize this diffusion-dependent, off-resonance effect. Dependence on off-resonance frequency and power are also investigated. <B>3)<I> Development of a genetic MRI marker via in vivo magnetic nanoparticle synthesis.</I></B> This work seeks to provide a gene expression marker for MRI based on bacterial magnetosomes, tiny magnets produced by naturally occurring magnetotactic bacteria. Here, <I>magA</I> is expressed in a commonly used human cell line, 293FT, resulting in the production of magnetic, iron oxide nanoparticles by these cells. MRI shows these particles can be formed <I>in vivo</I> utilizing endogenous iron and can be used to visualize cells positive for <I>magA</I>. These results demonstrate <I>magA</I> alone is sufficient to produce magnetic nanoparticles and that it is an appropriate candidate for an MRI reporter gene.
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Advances in real-time phase-contrast flow MRI and multi-echo radial FLASHTan, Zhengguo 26 April 2016 (has links)
No description available.
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