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DR SAKHER-ALKHADERI
CONSULTANT RADIOLOGIST AMC
"Felix Bloch and Edward Purcell, both of whom were
awarded the Nobel Prize in 1952, discovered the
nuclear magnetic resonance (NMR) phenomenon
independently in 1946. In the period between 1950 and
1970, NMR was developed and used for chemical and
physical molecular analysis. In 1971 Raymond Damadian
showed that the nuclear magnetic relaxation times of
tissues and tumors differed, thus motivating
scientists to consider magnetic resonance for the
detection of diseases. Dr. Damadian and his team
spent the next seven years diligently designing and
creating the first MRI machine for medical imaging of
the human body."
MRI HISTORY
FONAR introduced the world's first commercial MRI (a whole-body MRI scanner)
in 1980, and went public in 1981.
The first MRI images produced by the machine .
1977
Modern MRI
TYPES OF MRI
The OPEN MRI's started to come into production . The initial intent was to provide a
tool to perform the MRI diagnostic testing for patients that were a) Claustrophobic
or 2) Too obese to fit into the Closed models.
Neutral Flexion
Dynamic MRI
Surface Coils.
Surface coils are designed to provide a very high RF sensitivity over a small reg
interest. These coils are often single or multi-turn loops which are placed direct
the anatomy of interest. The size of these coils can be optimized for the specifi
region of interest.
MRI : WHAT IS
THE EXACT
PRINCIPLE
RADIOFEQUENCY
TURN OFF
Camera
SO TO GET AN IMAGE WE NEED
THE SIGNAL IS DISPLAYED ON GREY SCALE
AND ACCORDING TO THE RELAXATION TIME WE GET
Dark signal on all sequences
SPECIAL MRI SEQUENCES
 Diffusion weighted imaging (DWI) is a form of MR
imaging based upon measuring the random
Brownian motion of water molecules within a
voxel of tissue. The relationship between histology
and diffusion is complex, however generally
densely cellular tissues or those with cellular
swelling exhibit lower diffusion coefficients, and
thus diffusion is particularly useful in tumour
characterisation and cerebral ischaemia.
 DW imaging has a major role in the following clinical
situations 3-5:
 early identification of ischemic stroke
 differentiation of acute from chronic stroke
 differentiation of acute stroke from other stroke mimics
 differentiation of epidermoid cyst from arachnoid cyst
 differentiation of abscess from necrotic tumors
 assessment of cortical lesions in CJD
 differentiation of herpes encephalitis from diffuse temporal
gliomas
 assessment of the extent of diffuse axonal injury
 grading of gliomas and meningiomas (need further study)
 assessment of active demyelination
EPIDERMOID CYST
Functional magnetic resonance
imaging or functional MRI (fMRI) is
a functional neuroimaging procedure
using MRItechnology that measures brain activity by
detecting associated changes in blood flow.[1][2] This
technique relies on the fact that cerebral blood flow
and neuronal activation are coupled. When an area of
the brain is in use, blood flow to that region also
increases.
The primary form of fMRI uses the blood-oxygen-level
dependent (BOLD) contrast,[3] discovered by Seiji
Ogawa. This is a type of specialized brain and body
scan used to map neural activity in the brain or spinal
cord of humans or other animals by imaging the
change in blood flow (hemodynamic response)
related to energy use by brain cells.
MRI
SPECTROSCOPY
The basic principle that enables MR
spectroscopy (MRS) is the electron
cloud around an atom that shields the
nucleus from the magnetic field to a
greater or lesser degree. This naturally
results in slightly resonant frequencies,
which in turn return a slightly different
signal.
MR spectroscopy
MR spectroscopy (MRS)
Hunter's angle
lactate peak: resonates at 1.3 ppm
lipids peak: resonate at 1.3 ppm
alanine peak: resonates at 1.48 ppm
N-acetylaspartate (NAA) peak: resonates at 2.0
glutamine-glutamate peak: resonate at 2.2-2.4 ppm
gamma-aminobutyric acid (GABA) peak: resonate at
2.2-2.4 ppm
citrate peak: resonates at 2.6 ppm
creatine peak: resonates at 3.0 ppm
choline peak: resonates at 3.2 ppm
myo-inositol peak: resonates at 3.5 ppm
 Magnetic resonance elastography (MRE) is a non-
invasive medical imaging technique that measures
the mechanical properties (stiffness) of soft tissues by
introducing shear waves and imaging their
propagation using MRI. Pathological tissues are often
stiffer than the surrounding normal tissue. For instance,
malignant breast tumors are much harder than
healthy fibro-glandular tissue. This characteristic has
been used by physicians for screening and diagnosis
of many diseases, through palpation. MRE calculates
the mechanical parameter as elicited by palpation,
in a non-invasive and objective way.
SUSEPTIBILTY WEIGHTED IMAGES ( SWI) FOR HEMORRHAGE
THE END

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Basics of MRI

  • 2. "Felix Bloch and Edward Purcell, both of whom were awarded the Nobel Prize in 1952, discovered the nuclear magnetic resonance (NMR) phenomenon independently in 1946. In the period between 1950 and 1970, NMR was developed and used for chemical and physical molecular analysis. In 1971 Raymond Damadian showed that the nuclear magnetic relaxation times of tissues and tumors differed, thus motivating scientists to consider magnetic resonance for the detection of diseases. Dr. Damadian and his team spent the next seven years diligently designing and creating the first MRI machine for medical imaging of the human body." MRI HISTORY FONAR introduced the world's first commercial MRI (a whole-body MRI scanner) in 1980, and went public in 1981.
  • 3.
  • 4. The first MRI images produced by the machine .
  • 7.
  • 8. The OPEN MRI's started to come into production . The initial intent was to provide a tool to perform the MRI diagnostic testing for patients that were a) Claustrophobic or 2) Too obese to fit into the Closed models.
  • 9.
  • 10.
  • 12.
  • 13.
  • 14. Surface Coils. Surface coils are designed to provide a very high RF sensitivity over a small reg interest. These coils are often single or multi-turn loops which are placed direct the anatomy of interest. The size of these coils can be optimized for the specifi region of interest.
  • 15.
  • 16.
  • 17.
  • 18.
  • 19.
  • 20. MRI : WHAT IS THE EXACT PRINCIPLE
  • 21.
  • 22.
  • 23.
  • 24.
  • 25.
  • 27.
  • 30. SO TO GET AN IMAGE WE NEED
  • 31. THE SIGNAL IS DISPLAYED ON GREY SCALE
  • 32. AND ACCORDING TO THE RELAXATION TIME WE GET
  • 33.
  • 34.
  • 35.
  • 36.
  • 37.
  • 38.
  • 39.
  • 40. Dark signal on all sequences
  • 41.
  • 42.
  • 44.
  • 45.
  • 46.
  • 47.
  • 48.
  • 49.
  • 50.  Diffusion weighted imaging (DWI) is a form of MR imaging based upon measuring the random Brownian motion of water molecules within a voxel of tissue. The relationship between histology and diffusion is complex, however generally densely cellular tissues or those with cellular swelling exhibit lower diffusion coefficients, and thus diffusion is particularly useful in tumour characterisation and cerebral ischaemia.
  • 51.  DW imaging has a major role in the following clinical situations 3-5:  early identification of ischemic stroke  differentiation of acute from chronic stroke  differentiation of acute stroke from other stroke mimics  differentiation of epidermoid cyst from arachnoid cyst  differentiation of abscess from necrotic tumors  assessment of cortical lesions in CJD  differentiation of herpes encephalitis from diffuse temporal gliomas  assessment of the extent of diffuse axonal injury  grading of gliomas and meningiomas (need further study)  assessment of active demyelination
  • 52.
  • 54.
  • 55.
  • 56.
  • 57. Functional magnetic resonance imaging or functional MRI (fMRI) is a functional neuroimaging procedure using MRItechnology that measures brain activity by detecting associated changes in blood flow.[1][2] This technique relies on the fact that cerebral blood flow and neuronal activation are coupled. When an area of the brain is in use, blood flow to that region also increases. The primary form of fMRI uses the blood-oxygen-level dependent (BOLD) contrast,[3] discovered by Seiji Ogawa. This is a type of specialized brain and body scan used to map neural activity in the brain or spinal cord of humans or other animals by imaging the change in blood flow (hemodynamic response) related to energy use by brain cells.
  • 58.
  • 59. MRI SPECTROSCOPY The basic principle that enables MR spectroscopy (MRS) is the electron cloud around an atom that shields the nucleus from the magnetic field to a greater or lesser degree. This naturally results in slightly resonant frequencies, which in turn return a slightly different signal.
  • 60. MR spectroscopy MR spectroscopy (MRS) Hunter's angle lactate peak: resonates at 1.3 ppm lipids peak: resonate at 1.3 ppm alanine peak: resonates at 1.48 ppm N-acetylaspartate (NAA) peak: resonates at 2.0 glutamine-glutamate peak: resonate at 2.2-2.4 ppm gamma-aminobutyric acid (GABA) peak: resonate at 2.2-2.4 ppm citrate peak: resonates at 2.6 ppm creatine peak: resonates at 3.0 ppm choline peak: resonates at 3.2 ppm myo-inositol peak: resonates at 3.5 ppm
  • 61.
  • 62.
  • 63.
  • 64.  Magnetic resonance elastography (MRE) is a non- invasive medical imaging technique that measures the mechanical properties (stiffness) of soft tissues by introducing shear waves and imaging their propagation using MRI. Pathological tissues are often stiffer than the surrounding normal tissue. For instance, malignant breast tumors are much harder than healthy fibro-glandular tissue. This characteristic has been used by physicians for screening and diagnosis of many diseases, through palpation. MRE calculates the mechanical parameter as elicited by palpation, in a non-invasive and objective way.
  • 65.
  • 66. SUSEPTIBILTY WEIGHTED IMAGES ( SWI) FOR HEMORRHAGE

Editor's Notes

  1. On july,3,1977 the first human scan by Dr damadian