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Saturation
 
In MR, saturation is a nonequilibrium state with no net magnetization. The same amount of nuclear spins is aligned against and with the magnetic field. Saturation methods like FatSat, SPIR etc., work with a frequency selective saturation pulse for a specific chemical shift applied before the actual sequence starts. This saturation pulse adjusts the magnetization from tissue components to zero. The hydrogen nuclei of fat and water resonate at different frequencies, which makes it possible to excite just the fat with repeatedly applying RF pulses at the Larmor frequency with interpulse times compared to T1. The resulting signal is then destroyed with a gradient pulse (Spoiler Gradient Pulse). Fat is the chemical compound to be saturated at a fat saturation sequence. When the actual sequence follows, (e.g., a spin echo sequence) the unwanted suppressed component will not resonate.

See also Saturation Recovery.
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    • Baseline
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    • Spectral Selection Attenuated Inversion Recovery
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Manganese ChlorideInfoSheet: - Contrast Agents - 
Intro, Overview, 
Characteristics, 
Types of, 
etc.
 
Manganese chloride (MnCl2) is used as an oral contrast agent (LumenHance®) for MRI of the abdomen and/or pelvis. MnCl2 has also been used in magnetic resonance imaging of animals to maximize the contrast of different tissues e.g. in mice and crayfish with different injection methods. Caused by the hepatic uptake, manganese chloride has potential as a hepatobiliary contrast agent.
Manganese chloride is produced by the reaction of hydrochloric acid with manganese oxide or manganese carbonate. In an aqueous solution, manganese chloride can serve as phantom fluid, used for e.g. the daily quality assurance.

See also Classifications, Characteristics, etc.
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Further Reading:
  Basics:
Manganese-based MRI contrast agents: past, present and future
Friday, 4 November 2011   by www.ncbi.nlm.nih.gov    
Longitudinal MRI contrast enhanced monitoring of early tumour development with manganese chloride (MnCl2) and superparamagnetic iron oxide nanoparticles (SPIOs) in a CT1258 based in vivo model of prostate cancer
Wednesday, 11 July 2012   by www.biomedcentral.com    
In vitro evaluation of a manganese chloride phantom-based MRI technique for quantitative determination of lumbar intervertebral disc composition and condition
Friday, 11 March 2011   by www.ncbi.nlm.nih.gov    
  News & More:
Study compares effect of food intake on manganese-based MRI contrast agent absorption
Saturday, 3 December 2022   by www.itnonline.com    
Carbonized paramagnetic complexes of Mn (II) as contrast agents for precise magnetic resonance imaging of sub-millimeter-sized orthotopic tumors
Monday, 11 April 2022   by www.nature.com    
Gold-manganese nanoparticles for targeted diagnostic and imaging
Thursday, 12 November 2015   by www.nanowerk.com    
MRI Resources 
Calculation - Software - Raman Spectroscopy - Contrast Agents - Online Books - Most Wanted
 
Flow QuantificationInfoSheet: - Sequences - 
Intro, 
Overview, 
Types of, 
etc.
 
Quantification relies on inflow effects or on spin phase effects and therefore on quantifying the phase shifts of moving tissues relative to stationary tissues.
With properly designed pulse sequences (see phase contrast sequence) the pixel by pixel phase represents a map of the velocities measured in the imaging plane. Spin phase effect-based flow quantification schemes use pulse sequences specifically designed so that the phase angle in a pixel obtained upon measuring the signal is proportional to the velocity. As the relation of the phase angle to the velocity is defined by the gradient amplitudes and the gradient switch-on times, which are known, velocity can be determined quantitatively on a pixel-by-pixel basis. Once, this velocity is known, the flow in a vessel can be determined by multiplying the pixel area with the pixel velocity. Summing this quantity for all pixels inside a vessel results in a flow volume, which is measured, e.g. in ml/sec.
Flow related enhancement-based flow quantification techniques (entry phenomena) work because spins in a section perpendicular to the vessel of interest are labeled with some radio frequency RF pulse. Positional readout of the tagged spins some time T later will show the distance D they have traveled.
For constant flow, the velocity v is obtained by dividing the distance D by the time T : v = D/T. Variations of this basic principle have been proposed to measure flow, but the standard methods to measure velocity and flow use the spin phase effect.
Cardiac MRI sequences are used to encode images with velocity information. These pulse sequences permit quantification of flow-related physiologic data, such as blood flow in the aorta or pulmonary arteries and the peak velocity across stenotic valves.
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Searchterm 'mr methods' was also found in the following services: 
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Magnetic Field Mapping
 
The mapping of the magnetic field by measuring or imaging the spatial distribution of magnetic field strength, can be performed by scanning with a probe and handles a large range of field strengths, but is slow and tedious. Accurate field maps can be made by measuring the Larmor frequency as a function of position.
The field must be homogeneous enough to allow MR imaging to be performed, than the magnetic field can be mapped by different methods.
1. The adaptation of chemical shift imaging.
2. The faster one measures the change in signal phase in an image obtained with a gradient echo pulse sequence resulting from a change in echo time TE, which is proportional to the local field strength.
Also useful is a spin echo pulse sequence with data collection from two time locations of the readout gradient and the data acquisition interval, where each having a known shift of the acquisition center away from the spin echo.
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Further Reading:
  News & More:
sPHENIX assembly update: magnet mapped, detectors prepared
Friday, 23 December 2022   by www.eurekalert.org    
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Absorption and Emission - Cochlear Implant - Shoulder MRI - Musculoskeletal and Joint MRI - Corporations - Pregnancy
 
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