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Optic Neuritis as an Early Sign of Multiple Sclerosis

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This patient presented with

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left eye blurred vision.

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This was the first neurologic

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symptom of the patient.

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For orbital imaging,

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we rely most heavily on coronal sequences with

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T1-weighted scans to look for masses,

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T2-weighted scans to look at the optic nerve

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and postgadolinium-enhanced scans

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to characterize the lesion.

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On this T2-weighted scan,

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one can see that the left optic nerve

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is brighter in signal intensity

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than the right optic nerve.

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Let's look at the right optic nerve.

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What you see is fat-suppressed

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fat dark in signal intensity.

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Then you see the edge

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with the fat,

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which is the edge of the optic nerve sheath.

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Between the optic nerve and the optic

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nerve sheath, we have bright CSF.

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And then centrally,

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we have the optic nerve itself,

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which, because it's a white matter tract,

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has the same signal intensity as the

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white matter of the frontal lobe.

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Now, on the left side,

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we have an indistinct optic

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nerve sheath complex.

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It all looks like the same signal intensity with

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no distinction between CSF and the optic nerve.

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And that's because the optic nerve here

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is bright in signal intensity,

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brighter than the white matter.

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This is abnormal.

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If we look on the corresponding postgad fatsat

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T1-weight scan to the far right,

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we see that indeed,

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this optic nerve is enhancing compared to

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the non-enhancing right optic nerve.

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Let me just magnify this even further.

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So here we have an enlarged optic nerve sheath

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complex with a bright optic nerve.

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And on the post gadolinium-enhanced scan,

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again,

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you can see that that optic nerve

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is showing contrast enhancement.

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These are the image characteristics of optic

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neuritis. Is there a differential diagnosis?

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There's always a differential diagnosis,

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and it doesn't tell us what the etiology

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of the optic neuritis is.

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There are viral optic neuritis.

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There's autoimmune optic neuritis,

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there's infectious inflammatory optic neuritis.

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There's all different varieties

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of optic neuritis,

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including collagen vascular disease we could

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even have. And this. Ischemic optic neuropathy,

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which actually is the most common cause of optic

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neuropathy is small vessel ischemic

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disease in the elderly.

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However,

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in a young patient

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with an enhancing and enlarged optic nerve,

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we would raise the possibility of autoimmune

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idiopathic optic neuritis.

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This patient had a single symptom

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just left optic neuritis. So therefore,

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this patient could be said to have clinically

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isolated syndrome, a single neurologic event.

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What one wants to do in that situation is to

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scan the patient's brain to see whether

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there are any demyelinating plaques,

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which could suggest that this patient

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will progress to multiple sclerosis.

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In point of fact,

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this patient does indeed have some

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subcortical white matter lesions

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that are seen here

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in the frontal lobes. Now,

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this is a nonspecific pattern and doesn't yet

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fulfill McDonald criteria unless and until we

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also have periventricular white matter lesions,

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juxtacortical white matter lesions,

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or

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spinal cord lesions. If, on the other hand,

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we're using the magnums criteria and we have

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optic neuritis and juxtaportical

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white matter lesions,

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we would have fulfilled the magnums

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criteria for multiple sclerosis.

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Given that the patient only has

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a solitary neurologic event,

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this would still be called clinically

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isolated syndrome.

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But by virtue of the white matter

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lesions in the brain,

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it would have a higher rate of conversion over

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the course of time to a final ultimate

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diagnosis of multiple sclerosis.

Report

Description

Faculty

David M Yousem, MD, MBA

Professor of Radiology, Vice Chairman and Associate Dean

Johns Hopkins University

Tags

Neuroradiology

Metabolic

MRI

Idiopathic

Brain

Acquired/Developmental

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