Interactive Transcript
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There is a lot of research being
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performed on multiple sclerosis.
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There's a lot of NIH-sponsored grants on
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multiple sclerosis because, as I said,
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this is the most common
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neurodegenerative disorder
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of young adults.
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And a lot of the research has focused on
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different MR Techniques and what MR.
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Techniques predict the disability
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associated with the patient who
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has multiple sclerosis.
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So we're going to look at a few of these
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research pulse sequences just to wet
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your appetite for what's coming down the
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pike for clinical evaluation as well.
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So I mentioned that seven Tesla imaging
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is quite often performed in the research
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world for multiple sclerosis.
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And we saw some seven Tesla
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brilliant flare imaging.
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Seven Tesla scanners have been approved
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for clinical evaluation of the brain,
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and some sites will be employing seven
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Tesla imaging in their clinical realm.
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However,
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with respect to research protocols,
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I want to emphasize susceptibility
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weighted imaging.
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We are all comfortable now at 1.5 T and
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three T with susceptibility-weighted
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imaging to look for blood products.
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And we note that it also highlights the
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venous system because of the presence of
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deoxyhemoglobin within the veins that
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make the blood vessels dark.
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Well, this,
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coupled with the knowledge that multiple
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sclerosis is a perivenular
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demyelinating disorder,
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allows us to see the active plaques and
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the demyelination around these veins
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even better. So, as you see,
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there are already arrows on here showing
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the dark signal intensity linear veins
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with the demyelination around it.
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But let's just look at this case
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where we have the vein
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and the demyelination. This was present,
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and we saw that on the flare imaging,
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but with SWI,
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we see the veins much better.
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And I think this is a beautiful example
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here of the linear vein surrounded by
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the bright signal demyelination on an
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SWI T2-weighted pulse sequence.
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And this is demonstrated additionally
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on the images
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on the right. Now,
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multiple sclerosis in general
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does not show hemorrhage.
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When we have hemorrhage in association
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with a demyelinating plaque,
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we will think of a different
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differential diagnosis.
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So that's another value of SWI,
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is that we usually do not associate
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hemorrhage with demyelination
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from multiple sclerosis.
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So seven Tesla susceptibility
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weighted imaging. Now,
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others have utilized the susceptibility
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weighted imaging to analyze the iron
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content within the brain and the total
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iron burden of demyelinating plaques.
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So, in this example,
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we have what is known as quantitative
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susceptibility.
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Mapping or QSM,
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and it is a way of grading the degree of
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iron deposition in the brain
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from the demyelination.
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And these are just different
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pulse sequences,
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initially with the flare and with T1
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way and post gadolinium-enhanced scan,
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but down below in DE and F in this
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article by Ravi Menon, we're looking at
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the susceptibility aid scan and we are
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now quantifying the degree of iron
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deposition in the brain from this
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demyelinating disorder of
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multiple sclerosis.
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What he has found is that there is
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indeed increased iron deposition in gray
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matter as well as white matter compared
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to in patients with multiple sclerosis
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compared to controls,
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and that that amount of iron deposition
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correlates best with the expanded
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disability scale for patients with
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multiple sclerosis. So again,
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the idea being how can we correlate
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imaging findings to the degree of
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disability of the patient who
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has multiple sclerosis?
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Other people have used the
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combination of the QSM,
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the quantitative iron content
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with T2* effects,
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as well as gadolinium enhancement to try
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to define the different types of plaques
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that occur in multiple sclerosis,
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including early active plaque,
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late active plaque,
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or chronic plaques that are
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stable if you will.
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And this is one example of a research
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group looking at various combinations to
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define whether a plaque is early active,
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maybe requiring pharmaceutical
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intervention,
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late active on its way to dormancy
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versus chronic plaques.
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And here you can see the different types
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of imaging that is being performed.
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You have the T1-weighted
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post-gadolinium T2-weight scan and
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then the quantitative susceptibility
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mapping and R2* imaging that is
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demonstrating early nodular plaque
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versus early peripheral enhancing plaque
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and the fact that the early nodular
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pattern shows myelin breakdown,
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whereas the peripheral plaque shows some
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myelin degradation but
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not active breakdown.
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The late plaques generally are not going
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to show contrast enhancement seen in the
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upper left image on post-gadolinium
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enhanced scan.
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And you also see that there is some iron
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deposition that's occurring in the late
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plaques and some of the iron content may
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be either in a rim fashion or
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in a more solid fashion.
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So these are just different research
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techniques to try to define stages of
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demyelination within a patient's scan
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who has multiple sclerosis.
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