Interactive Transcript
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This is a young adult woman who had multiple
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episodes of tingling and paresthesias,
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initially in the upper extremity and
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then also in the lower extremity.
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As we scroll the sagittal STIR sequences,
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we see that there are areas of high signal
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intensity in the cervical spinal cord
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opposite C4, C5, C6,
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as well as an additional lesion at T2.
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What's different about these lesions is that, by and large,
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they are not causing expansion of the spinal cord.
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This T2 lesion may have a little bit of widening.
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These are single-segment lesions.
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When we extend our imaging to
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the thoracic spinal cord,
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we see additional areas of high signal intensity
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without cord expansion in the mid thoracic region,
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as well as the lower thoracic spinal cord.
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On post-gadolinium-enhanced imaging,
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there is no evidence of spinal cord enhancement
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that corresponds to these lesions,
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which would make it neoplasm much less likely.
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So what's in our differential diagnosis?
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You might think about neoplastic category,
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except that the cord really isn't expanded,
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and is not showing contrast enhancement.
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We don't see very much in the way of
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degenerative change. So at this juncture,
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we probably go with the next most common
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category of disease in the spinal cord,
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and that is demyelination,
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which is under our eye for idiopathic in our
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VITAMIN C and D. So we would think, "Oh,
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could this be a vascular lesion?"
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No. Could it be an infectious lesion?
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Unlikely. Could it be trauma? No.
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Acquired? No. Metabolic? Unlikely.
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Idiopathic is where we have demyelinating
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disorders. Neoplasm? Definitely not. Congenital?
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No. And drug-related? No.
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So this is indeed multiple sclerosis of the
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spinal cord with multiple lesions without cord
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expansion and without demonstrating
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contrast enhancement. As an aside,
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you're seeing some venous vascular malformations
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or hemangiomas of bone showing enhancement,
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but that cord lesion is not enhancing.
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Fortunately, we have the brain MRI scan.
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So isolated spinal cord demyelination with
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multiple sclerosis is very unusual.
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You can get it with neuromyelitis optica.
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So we would next scan the brain.
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As we scan the brain with our sagittal
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FLAIR imaging,
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we see multiple periventricular and
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subcortical white matter lesions
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bilaterally in the brain.
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The posterior fossa seems to be spared.
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We'd have to get out our T2-weighted
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imaging and look at the posterior fossa.
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So by McDonald criteria,
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we have periventricular and juxtaportical and
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spinal cord white matter lesions that would
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fulfill the dissemination in space
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criteria for multiple sclerosis.
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We'd have to look for enhancing lesions or new
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lesions in order to fulfill the dissemination
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in time criteria for multiple sclerosis.
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So within the demyelinating category,
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multiple sclerosis and neuromyelitis optica are
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the most common of the lesions affecting the
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spinal cord, and they are indeed intradural
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intramedullary lesions.
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