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 'Selective Excitation' 
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Result : Searchterm 'Selective Excitation' found in 2 terms [] and 16 definitions [], (+ 5 Boolean[] results
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Spin Echo Sequence for Spatial LocalizationInfoSheet: - Sequences - 
Intro, 
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etc.MRI Resource Directory:
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(DEPTH) A sequence with multiple RF pulses to enable acquiring data from only selected regions.
See Depth Pulses, Volume Selective Excitation, Depth Resolved Spectroscopy.
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Time of Flight AngiographyInfoSheet: - Sequences - 
Intro, 
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etc.MRI Resource Directory:
 - MRA -
 
(TOF) The time of flight angiography is used for the imaging of vessels. Usually the sequence type is a gradient echo sequences with short TR, acquired with slices perpendicular to the direction of blood flow.
The source of diverse flow effects is the difference between the unsaturated and presaturated spins and creates a bright vascular image without the invasive use of contrast media. Flowing blood moves unsaturated spins from outside the slice into the imaging plane. These completely relaxed spins have full equilibrium magnetization and produce (when entering the imaging plane) a much higher signal than stationary spins if a gradient echo sequence is generated. This flow related enhancement is also referred to as entry slice phenomenon, or inflow enhancement.
Performing a presaturation slab on one side parallel to the slice can selectively destroy the MR signal from the in-flowing blood from this side of the slice. This allows the technique to be flow direction sensitive and to separate arteriograms or venograms. When the local magnetization of moving blood is selectively altered in a region, e.g. by selective excitation, it carries the altered magnetization with it when it moves, thus tagging the selected region for times on the order of the relaxation times.
For maximum flow signal, a complete new part of blood has to enter the slice every repetition (TR) period, which makes time of flight angiography sensitive to flow-velocity. The choice of TR and slice thickness should be appropriate to the expected flow-velocities because even small changes in slice thickness influences the performance of the TOF sequence. The use of sequential 2 dimensional Fourier transformation (2DFT) slices, 3DFT slabs, or multiple 3D slabs (chunks) are depending on the coverage required and the range of flow-velocities.
3D TOF MRA is routinely used for evaluating the Circle of Willis.

See also Magnetic Resonance Angiography and Contrast Enhanced Magnetic Resonance Angiography.
 
Images, Movies, Sliders:
 TOF-MRA Circle of Willis Inverted MIP  Open this link in a new window
    

 Circle of Willis, Time of Flight, MIP  Open this link in a new window
    
SlidersSliders Overview

 
Radiology-tip.comradCT Angiography,  Coronary Angiogram
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Medical-Ultrasound-Imaging.comColor Power Angio,  Doppler Ultrasound
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• View the DATABASE results for 'Time of Flight Angiography' (11).Open this link in a new window

 
Further Reading:
  Basics:
MR–ANGIOGRAPHY(.pdf)
  News & More:
Magnetic resonance angiography: current status and future directions
Wednesday, 9 March 2011   by www.jcmr-online.com    
MRI Resources 
NMR - Image Quality - Blood Flow Imaging - Education - PACS - Brain MRI
 
Volume Excitation Stimulated Echoes
 
(VEST) The 'Volume Excitation Stimulated Echoes' sequence is a method similar to point resolved spectroscopy with stimulated echoes and volume selective excitation.
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Chemical Shift ImagingInfoSheet: - Sequences - 
Intro, 
Overview, 
Types of, 
etc.MRI Resource Directory:
 - Spectroscopy pool -
 
(CSI) Chemical shift imaging is an extension of MR spectroscopy, allowing metabolite information to be measured in an extended region and to add the chemical analysis of body tissues to the potential clinical utility of Magnetic Resonance. The spatial location is phase encoded and a spectrum is recorded at each phase encoding step to allow the spectra acquisition in a number of volumes covering the whole sample. CSI provides mapping of chemical shifts, analog to individual spectral lines or groups of lines.
Spatial resolution can be in one, two or three dimensions, but with long acquisition times od full 3D CSI. Commonly a slice-selected 2D acquisition is used. The chemical composition of each voxel is represented by spectra, or as an image in which the signal intensity depends on the concentration of an individual metabolite. Alternatively frequency-selective pulses excite only a single spectral component.
There are several methods of performing chemical shift imaging, e.g. the inversion recovery method, chemical shift selective imaging sequence, chemical shift insensitive slice selective RF pulse, the saturation method, spatial and chemical shift encoded excitation and quantitative chemical shift imaging.

See also Magnetic Resonance Spectroscopy.
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• View the DATABASE results for 'Chemical Shift Imaging' (6).Open this link in a new window

 
Further Reading:
  Basics:
1H MR Spectroscopy and Chemical Shift Imaging of the In Vivo Brain at 7 Tesla
Sunday, 26 November 2006   by tobias-lib.uni-tuebingen.de    
MRI evaluation of fatty liver in day to day practice: Quantitative and qualitative methods
Wednesday, 3 September 2014   by www.sciencedirect.com    
  News & More:
Spin echoes, CPMG and T2 relaxation - Introductory NMR & MRI from Magritek
2013   by www.azom.com    
mDIXON being developed to simplify and accelerate liver MRI
September 2010   by incenter.medical.philips.com    
MRI Resources 
MR Myelography - Collections - Spine MRI - Corporations - Research Labs - Equipment
 
Frequency Selective RF Pulse
 
A RF pulse containing energy only within a specified frequency range. Usually used for slice excitation or for selective saturation pulses.
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