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MS Plaques

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Let's look at some of the imaging of multiple

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sclerosis and the plaques

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that are associated with it.

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So on your left-hand side,

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you have something which is a

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little bit anachronistic,

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and that is a proton density-weighted scan.

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As I mentioned,

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there are multiple research programs that are

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using the combination of proton density

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weighted imaging and T2-weighted imaging to

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do volumetric analysis of multiple

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sclerosis plaques.

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Because proton density-weight imaging and T

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two-weighted imaging come as a dual echo

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sequence, you don't show motion artifact,

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which would cause a little bit of offset when

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you're doing volumetric imaging. For MS.

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Plaque volume.

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On the proton density-weight scan,

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you can see that the CSF is slightly

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low in signal intensity,

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but the demyelination is bright.

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So by that,

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I mean that this CSF space is a little bit

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darker in signal intensity than the

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Demyelination on a proton

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density-weighted scan.

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Contrast that with your flare scan

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on your right-hand side,

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in which case you see a very dark CSF sulcus,

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but very nicely demonstrated the contrast

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with the white matter lesions.

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So these would be classified as

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periventricular white matter disease,

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and as we get close to the cortex,

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we would have juxtacortical lesions on the

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flare scan being demonstrated here,

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this lesion is probably at the top of the

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lateral ventricle and so would really be

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classified more as a periventricular lesion.

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So we've seen juxtacortical lesions,

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and we've seen periventricular lesions.

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The other areas that we include in the four

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locations of the McDonald criteria are the

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infratentorial space and the spine.

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Within the infratentorial space,

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we include those lesions that are in the brain

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stem as well as those out in the

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periphery of the cerebellum.

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This is a lesion in the middle cerebellar

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peduncle classified as infratentorial

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in location. However, as I said,

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it's important to look at the

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periphery of the brain stem,

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because quite often you see small lesions on

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the surface of the brain stem that will be

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classified as demyelinating plaques

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fulfilling infratentorial location.

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Those white matter lesions out in the

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periphery of the cerebellum are better seen

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on T2-weighted scan than flare scan,

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and that is why we emphasize the T2-weight

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scan for infratentorial evaluation.

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To the right, we see spinal cord lesions.

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The spinal cord lesions of multiple sclerosis

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usually represent one to two segment disease.

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These are not the long segment disease.

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So this lesion, by segment,

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we're talking about two C, three C, four,

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each of these being a segment of the spine.

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Notice that the white matter lesions here are

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separated as smaller lesions that

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span one to two segments,

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not longitudinally

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extensive white matter lesions.

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Longitudinally extensive white matter lesions

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are what we will see more commonly in

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neuromyelitis optica spectrum disorder and in

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idiopathic acquired transverse myelitis.

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Just as in the brain.

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We do the post-gad scans in the spine

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to look for enhancing plaques,

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and these enhancing plaques can be seen

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showing peripheral enhancement or

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solid contrast enhancement.

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On the post-gad T1-weighted scans,

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we use traditional Spin-echo

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T1-weighted scans.

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Some people are using Vibe scans because you

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can get thinner sections. In some cases,

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it may show the periphery

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of the spinal cord better.

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So you have your choice there between spine

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echo T1-weight scans versus the

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Vibe T1-weight technique.

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Sagittal flare scans are critically important

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because they show the white marrow

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lesions very nicely,

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as well as defining what I had described

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previously as your colossal

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septal interface lesion.

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So this is at the periphery under surface

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of the corpus callosum seen here,

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and this is the area of the septum polysum.

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And hence we have that area called

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the colossal septal interface.

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And that is relatively specific for multiple

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sclerosis as opposed to other

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demyelinating disorders.

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As we go off in the periphery again,

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we see more white matter lesions and you may

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see some out in the peripheral white matter

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again. And this one just off midline.

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We're seeing the pineal gland and the

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tectoplate here. We're just off midline,

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a very nicely demonstrated lesion at the

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colossal septal interface with respect

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to gadolinium enhancement.

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Here we have a patient who has white matter

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lesions in what appears to be the cortex

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going all the way to the periphery.

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So this is a cortical involvement.

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And for that McDonald's

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criteria,

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as well as juxtaportical involvement on

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post-gadolinium enhanced scan again,

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we see the various types of contrast-enhancing

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demyelinating plaques that can occur

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all on one single post-gad image.

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That's why I keep this slide.

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Have the one that is a complete rim

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of enhancement.

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We have the open rim

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or arcs of enhancement,

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we have a more solid contrast enhancement

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and we have some more linear

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enhancing plaques.

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So multiple different of gadolinium

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enhancement by multiple sclerosis plaques.

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For dissemination in time,

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we need to see a patient show either enhancing

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plaques and none-enhancing plaques

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on the same study,

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or plaques that appear and or go

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away on sequential studies.

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So this is the same patient and what one sees

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on this patient is a flare

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scan to the far left.

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On this flare scan, we have the Sylvian Fissure

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and we have the demyelinating plaque.

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On the follow-up scan,

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we have the Sylvian Fissure and you notice

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that the plaque has gone away.

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So this satisfies dissemination in time.

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On sequential imaging,

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you notice that this patient also had a

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peripheral enhancing plaque which no

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longer shows contrast enhancement.

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If we have enhancing plaques and none

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enhancing plaques on the same study,

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we fulfill dissemination in time.

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However, in this case,

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this was the follow-up scan showing that the

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plaque enhancement had resolved. Similarly,

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on the far right-hand side,

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we have a patient who has a peripherally

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enhancing white matter demyelinating plaque,

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which on follow-up, if we track the psilci,

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has resolved another example of a large

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multiple sclerosis plaque, which,

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as you can see, changes in time.

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This was a three-month follow-up.

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So you see a large periventricular

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white matter plaque,

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which on the coronal image showed a sort

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of arc-like solid enhancement.

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On the follow-up scan,

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it decreases in size and it no longer

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shows contrast enhancement,

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fulfilling our dissemination

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in time criteria.

Report

Description

Faculty

David M Yousem, MD, MBA

Professor of Radiology, Vice Chairman and Associate Dean

Johns Hopkins University

Tags

Neuroradiology

Metabolic

MRI

Brain

Acquired/Developmental

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