Interactive Transcript
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This is a 56-year-old woman who presented
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with both motor and sensory symptoms in
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the lower extremity,
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as well as difficulty with urinary incontinence.
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We have a sagittal T1-weighted,
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a sagittal T2-weighted,
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and a sagittal FLAIR scan
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demonstrated here.
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What one sees is abnormal signal intensity
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within the spinal cord,
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which seems a little bit discontinuous
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but extends over at least four segments
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of the lower cervical and upper thoracic spine.
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I think this sagittal STIR image probably
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shows the abnormality the
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best with disease,
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which is extending at least over three
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vertebral body segments and seems to
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spare the upper cervical spine,
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but begins at approximately C7 and
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goes down to the T3 level.
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Let's look at the axial scans
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through this lower
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cervical region.
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So the initial cervical spine axial
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scans look pretty normal.
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And then we get to the C7 level where
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there is diffuse signal intensity
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abnormality throughout the spinal cord.
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So here you see that there is signal
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intensity abnormality that's involving
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the entirety of the spinal cord.
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Continuing to scroll more inferiorly
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below C7, T1,
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you see that there is continued
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abnormality in the spinal cord that
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affects the posterior cord.
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And then once again we have another area
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where greater involvement of the spinal
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cord more to the left than to the right
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occurs down in the T3 level.
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This is the postgadolinium enhanced scan
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where one can see that there is
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involvement of the spinal cord with
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more central contrast enhancement.
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So what we're seeing is,
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are these areas of spotty enhancement.
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This is 234567, T1, T2, T3,
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T4,
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where there is
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abnormal contrast enhancement over
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basically four thoracic levels.
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The cord abnormality, as you can see,
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corresponds to those areas from C7
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going down to T4 on the T2-weighted imaging.
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When one sees this,
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there is a very broad differential diagnosis.
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Effectively the patient is presenting
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with transverse myelitis.
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Transverse myelitis is not a
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specific diagnosis itself.
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It is a symptom complex and therefore it
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behooves us to try to identify
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the differential diagnosis.
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Is so in this situation,
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we would question whether or not the
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patient has any visual problems to suggest
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neuromyelitis optica spectrum disorder.
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Because this is longitudinally extensive
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involvement over multiple segments,
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this is not a pattern that would be
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typical of multiple sclerosis.
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We would also do the examination of the
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various this immunologic test to identify
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whether the patient has an autoimmune
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disorder, rheumatoid,
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a collagen vascular disorder, lupus,
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for example.
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CSF might be obtained to exclude an
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infectious cause of transverse myelitis.
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There are a number of viral etiologies,
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most commonly being CMV
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or Herpes myelitis,
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and we would also obviously check for HIV
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status because of the possibility
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of vacuolar myelopathy,
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which is associated with AIDS.
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Ischemic etiologies would be examined,
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but ischemic etiologies very rarely will
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show contrast enhancement
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of the spinal cord.
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Some programs are performing diffusion
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weighted imaging of the spinal cord which
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might help in diagnosing an ischemic
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transverse myelitis.
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Finally, we have the autoimmune disorders that
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can cause transverse myelitis.
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If we have the situation where we never
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identify an etiology for the
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transverse myelitis,
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you may see the term used IATM idiopathic
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acquired transverse myelitis.
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This has an intermediate prognosis.
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It is usually treated with
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immunosuppressives beginning
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with steroids,
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and the patient may resolve completely.
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However,
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one should consider that this may be the
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first episode of a polyphasic disorder
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such as acute disseminated
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encephalomyelitis with MDEM multifasic,
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multiphasic disseminated
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encephalomyelitis,
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or it may be a manifestation
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of the first episode.
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So the term that you may see is IATM
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Idiopathic Acquired Transverse Myelitis,
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which was the final diagnosis
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on this case.
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This is one of the selective demyelinating
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disorders of the spinal cord.
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