Interactive Transcript
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I mentioned previously, Horner syndrome,
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and I think it's important for me to define it.
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And this is due to damage to the sympathetic
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nervous system plexus,
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which is often associated with carotid dissection.
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Remember that the sympathetic nervous system plexus
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is just behind the carotid artery within the
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carotid sheath, so it's located posteriorly.
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The classic triad for Horner syndrome is meiosis,
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a small pupil, ptosis,
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a little bit of a lid drop, and facial
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anhidrosis, which is absence of sweating.
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So I've taken this well-known individual and
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identified for you the lid lag and the drop
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in the eyelid over the iris of the globe.
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And you see that it's covering a portion of the pupil.
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So that's the ptosis,
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the pupil itself is smaller in caliber on the side
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with the Horner syndrome versus the normal side.
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And then you have facial anhidrosis.
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So this is showing that this side is sweating,
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this side does not sweat.
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And that's anhidrosis, facial anhidrosis.
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Here's another example of Horner syndrome.
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The lid is down. It's covering part of the iris,
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more of the iris than the normal side.
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The pupil is smaller in size than the normal size.
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Miosis, ptosis, and facial anhidrosis.
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When you have Horner syndrome,
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most people would likely evaluate
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the patient with a CT angiogram (CTA).
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And the reason for that is because you really have
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to extend from intracranially to the cervical region
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down to the mediastinum and maybe
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even into the upper chest.
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And we just don't get that coverage very well with
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the various surface coils associated with MRI.
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So CTA to look also at the blood vessels and the MRI
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is good for looking at hypothalamic lesions,
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brainstem lesions, and cervical spinal cord lesions.
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But the initial diagnosis is
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usually made with CT angiogram (CTA).
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Sometimes you'll need a chest CT to look at the lung
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apex to see where there's a lesion at the lung apex
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which is pooching up and affecting the
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stellate ganglion at the C7-T1 level.
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Here we have a diagram looking at the neurons that
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are associated with Horner syndrome.
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We start off with the hypothalamus,
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and we see the first-order neuron is the one that
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goes down into the cervical spinal cord
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to the C6, C7, T1 level.
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So anywhere along the brainstem
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and the cervical spinal cord,
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you could affect the first-order neurons.
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You then have the ganglion here,
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which leads to the second-order neurons.
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These second-order neurons are the ones that transfer
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over the top of the lungs and therefore.
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A Pancoast tumor of the upper lung will affect the
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second-order neuron or the superior cervical
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ganglion that is associated with that.
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After the second-order neuron,
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you then have the crossing over
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into the carotid sheath.
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And these carotid sheath branches are part of the
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distal second-order neuron and the third-order
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neuron associated with the carotid artery.
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So here's our carotid artery,
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here's the carotid bifurcation,
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here's the superior cervical ganglion,
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usually at the C4 level and then the third-order
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neuron which goes up from the carotid sheath into
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the intracranial compartment once again and goes
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into the orbit and along the ophthalmic artery
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to lead to the pupillary dilator fibers.
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So the sympathetic nervous system plexus descends
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from the hypothalamus down to
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the thoracic spine T1,
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T2 level and then ascends via the carotid sheath
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up into the orbit to lead to the
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findings of miosis and ptosis.
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